US20050070838A1 - Intravascular spinal perfusion and cooling for use during aortic surgery - Google Patents

Intravascular spinal perfusion and cooling for use during aortic surgery Download PDF

Info

Publication number
US20050070838A1
US20050070838A1 US10/990,776 US99077604A US2005070838A1 US 20050070838 A1 US20050070838 A1 US 20050070838A1 US 99077604 A US99077604 A US 99077604A US 2005070838 A1 US2005070838 A1 US 2005070838A1
Authority
US
United States
Prior art keywords
aorta
perfusion
blood
intercostal
intercostal arteries
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Abandoned
Application number
US10/990,776
Inventor
Denise Barbut
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
CoAxia Inc
Original Assignee
CoAxia Inc
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by CoAxia Inc filed Critical CoAxia Inc
Priority to US10/990,776 priority Critical patent/US20050070838A1/en
Publication of US20050070838A1 publication Critical patent/US20050070838A1/en
Abandoned legal-status Critical Current

Links

Images

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61MDEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
    • A61M1/00Suction or pumping devices for medical purposes; Devices for carrying-off, for treatment of, or for carrying-over, body-liquids; Drainage systems
    • A61M1/36Other treatment of blood in a by-pass of the natural circulatory system, e.g. temperature adaptation, irradiation ; Extra-corporeal blood circuits
    • A61M1/3621Extra-corporeal blood circuits
    • A61M1/3653Interfaces between patient blood circulation and extra-corporal blood circuit
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61MDEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
    • A61M1/00Suction or pumping devices for medical purposes; Devices for carrying-off, for treatment of, or for carrying-over, body-liquids; Drainage systems
    • A61M1/36Other treatment of blood in a by-pass of the natural circulatory system, e.g. temperature adaptation, irradiation ; Extra-corporeal blood circuits
    • A61M1/3613Reperfusion, e.g. of the coronary vessels, e.g. retroperfusion
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61MDEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
    • A61M1/00Suction or pumping devices for medical purposes; Devices for carrying-off, for treatment of, or for carrying-over, body-liquids; Drainage systems
    • A61M1/36Other treatment of blood in a by-pass of the natural circulatory system, e.g. temperature adaptation, irradiation ; Extra-corporeal blood circuits
    • A61M1/3621Extra-corporeal blood circuits
    • A61M1/3653Interfaces between patient blood circulation and extra-corporal blood circuit
    • A61M1/3659Cannulae pertaining to extracorporeal circulation
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61MDEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
    • A61M1/00Suction or pumping devices for medical purposes; Devices for carrying-off, for treatment of, or for carrying-over, body-liquids; Drainage systems
    • A61M1/36Other treatment of blood in a by-pass of the natural circulatory system, e.g. temperature adaptation, irradiation ; Extra-corporeal blood circuits
    • A61M1/369Temperature treatment
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61MDEVICES FOR INTRODUCING MEDIA INTO, OR ONTO, THE BODY; DEVICES FOR TRANSDUCING BODY MEDIA OR FOR TAKING MEDIA FROM THE BODY; DEVICES FOR PRODUCING OR ENDING SLEEP OR STUPOR
    • A61M2205/00General characteristics of the apparatus
    • A61M2205/36General characteristics of the apparatus related to heating or cooling
    • A61M2205/3606General characteristics of the apparatus related to heating or cooling cooled

Definitions

  • the present invention relates generally to medical methods and devices, and more particularly, to methods and devices for cooling and perfusing the spinal vasculature of a patient during thoracoabdominal aortic surgery.
  • An exemplary procedure includes conventional aortic grafting, which involves clamping the aorta upstream from the damaged region to prevent blood loss at the surgical site, excising a cylindrical portion of the aorta encompassing the damaged region, and replacing the removed portion of the aorta with a graft. During this procedure, the intercostal arteries leading to the damaged region of the aorta are individually severed from the aorta.
  • the cessation of blood flow through the aorta causes spinal ischemia in about 10-15% of patients, due to the reduction or cessation of oxygenated blood within the spinal vasculature that would normally be supplied thereto by the intercostal arteries downstream from the clamped portion of the aorta. Because spinal ischemia can quickly lead to irreversible spinal tissue damage, a minimal amount of time is allowed to suture the intercostal arteries onto the graft. Often, when the intercostal arteries are severed from the aorta, none or very few of them are sutured onto the graft due to the time limitations.
  • the aortic clamp is removed after the graft is attached, thereby supplying oxygenated blood to the spinal vasculature via the unsevered intercostal arteries, albeit in a non-robust manner.
  • Spinal neurological damage is directly related to cross-clamp time and the number of severed intercostal arteries.
  • the intercostal arteries are sometimes integrally severed from the aorta, i.e., patches of the posterior wall of the aorta are excised, each of which carries several intercostal arteries.
  • the aortic patch can be sutured onto the graft, minimizing the amount of time it takes to connect the intercostal arteries to the aorta.
  • the invention provides single or multiple vessel perfusion assemblies and methods for selectively treating the spinal vasculature of a patient during thoracoabdominal surgery.
  • Methods performed in accordance with the present invention comprise perfusing the spinal vasculature with a medium by flowing a medium into the open ends of one or more intercostal arteries.
  • the intercostal arteries can be accessed by individually or integrally severing the intercostal arteries from the aorta, or alternatively, the intercostal arteries can be accessed through a puncture or slit within the wall of the aorta.
  • the medium is cooled to induce hypothermia within the spinal vasculature without cooling the rest of the body (selective spinal hypothermia).
  • the cooled medium can be composed of a biocompatible liquid, such as, e.g., a saline solution, that is flowed from an external source and is cooled.
  • the cooled medium can be composed of oxygenated blood that is shunted from an oxygenated blood filled cavity, such as the heart or proximal aorta upstream from the intercostal arteries and cooled.
  • the characteristics of the cooled medium such as, e.g., the temperature, flow rate and pressure of the medium is preferably controlled to maintain a viable environment for the spinal vasculature.
  • the methods of the present invention can be performed by employing any vessel perfusion assembly, but are preferably performed by flowing a medium into the plurality of intercostal arteries, which can be facilitated by employing single and multiple vessel perfusion assemblies, such as those described herein.
  • the multiple vessel perfusion assembly includes a branched conduit having a common portion, an inflow cannula formed at one end of the common portion and a plurality of outflow cannulae respectively formed at the other end of the common portion.
  • the branched conduit includes a lumen for conveyance of a medium therethrough.
  • the inflow cannula can comprise any tubular member configured to be inserted through the wall of the heart or proximal aorta
  • the outflow cannulae can comprise any tubular members configured to be inserted into the open ends of vessels.
  • the inflow cannula includes an inlet, and the outflow cannulae include outlets, which are in fluid communication with the lumen of the branched conduit.
  • insertion of the inflow cannula through the heart or aortic wall and respective insertion of the plurality of outflow cannulae into the open ends of the vessels provides flow of oxygenated blood from the heart or aorta into the vessels.
  • the branched multiple vessel perfusion assembly further includes a cooler for cooling the medium as it passes through the lumen of the branched conduit.
  • the multiple vessel perfusion assembly includes a conduit, an inflow cannula formed at one end of the conduit, and a perfusion chamber formed at the other end of the conduit.
  • the conduit includes a lumen
  • the inflow cannula and perfusion chamber respectively include an inlet and a substantially enclosed cavity, which are in fluid communication with the lumen of the conduit.
  • the perfusion chamber includes vessel engaging outlets, which are configured to securely receive the open ends of a plurality of integrally severed vessels (an aortic patch).
  • a single vessel perfusion assembly constructed in accordance with the present invention provides a means for flowing a medium into the open end of a vessel.
  • the single vessel perfusion assembly includes a conduit, an inflow cannula formed at one end of the conduit and an outflow cannula formed at the other end of the conduit.
  • the conduit includes a lumen for conveyance of a medium therethrough.
  • the inflow cannula includes an inlet, and the outflow cannula includes an outlet, which are in fluid communication with the lumen of the conduit.
  • the above multiple vessel perfusion assemblies can forego the employment of an inflow cannula.
  • a medium such as, e.g., a saline solution
  • the multiple vessel perfusion assemblies further include control devices for conditioning the medium to maintain a viable environment for the tissue to which the vessels lead.
  • a cooler and associated thermostat can be used to cool and control the temperature of the medium.
  • a pump and associated manometers can be used to control the flow rate and pressure of the medium.
  • FIG. 1 illustrates the systemic arterial circulation of a patient relevant to the present invention
  • FIG. 2 illustrates a first preferred embodiment of a multiple vessel perfusion assembly constructed in accordance with the present invention
  • FIG. 3 illustrates an alternative embodiment of the inflow cannula employed in the multiple vessel perfusion assembly of FIG. 2 ;
  • FIG. 4 illustrates a second preferred embodiment of a multiple vessel perfusion assembly constructed in accordance with the present invention
  • FIG. 5 illustrates a perfusion chamber employed in the multiple vessel perfusion assembly of FIG. 4 , which is particularly shown in a closed position;
  • FIG. 6 illustrates a perfusion chamber employed in the multiple vessel perfusion assembly of FIG. 4 , which is particularly shown in an open position;
  • FIG. 7 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of individually severed intercostal arteries by employing multiple vessel perfusion assembly of FIG. 2 ;
  • FIG. 8 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of integrally severed intercostal arteries by employing the multiple vessel perfusion assembly of FIG. 4 ;
  • FIG. 9 illustrates a preferred method of placing the open ends of a plurality of integrally severed intercostal arteries within the perfusion chamber of FIG. 5 ;
  • FIG. 10 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of intercostal arteries through a slit in the aorta;
  • FIG. 11 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of intercostal arteries through a puncture in the aorta;
  • FIG. 12 illustrates a preferred embodiment of a single vessel perfusion assembly constructed in accordance with the present invention.
  • FIG. 13 illustrates an embodiment of a single vessel perfusion assembly for use in the perfusion of a single intercostal artery.
  • Oxygenated blood (represented by arrows) from the heart 10 normally flows through the aorta 12 and into a multitude of intercostal arteries 14 , which branch off of the aorta 12 .
  • the oxygenated blood then flows from the intercostal arteries 14 into the spinal vasculature, i.e., the posterior spinal arteries 16 and the anterior spinal artery 18 (shown partially in phantom), where it is distributed to the spinal tissue.
  • the spinal vasculature is common to all of the intercostal arteries 14 , oxygenated blood can still be distributed to the entire spinal tissue even if the blood flow within some of the intercostal arteries 14 ceases.
  • Spinal ischemia will result, however, if the number of intercostal arteries 14 through which the blood flow is ceased is too great, which often occurs as a result of thoracoabdominal aortic surgery.
  • the branched multiple vessel perfusion assembly 100 can be used to shunt blood from the aorta 12 to a plurality of severed arteries, such as, e.g., severed intercostal arteries 14 .
  • the vessel perfusion assembly 100 generally includes a branched conduit 102 having a common portion 104 , an inflow cannula 108 formed at one end of the common portion 104 , and a plurality of outflow cannulae 110 respectively formed at the other end of the common portion 104 .
  • the inflow cannula 108 is configured to be inserted through the wall of the aorta 12 , and each of the outflow cannulae 110 are configured to be inserted into the open end of a severed intercostal artery, 14 .
  • the branched conduit 102 includes a blood lumen 112 extending therethrough.
  • the inflow cannula 108 includes an inlet 114
  • the each of the outflow cannulae 110 includes an outlet 116 .
  • the inlet 114 and outlets 116 are in fluid communication with the blood lumen 112 , such that blood entering the inlet 114 flows through the blood lumen 112 and exits the outlets 116 .
  • the branched conduit 102 is formed of elastomeric tubing.
  • the inflow cannula 108 includes a hollow needle 118 having a sharpened distal tip, such that the inflow cannula 108 can penetrate the wall of the aorta 12 .
  • the inlet 114 is located on the hollow needle 118 .
  • the inflow cannula 108 includes a blunt access tube 120 , which can be inserted inside the aorta 12 through a small incision or puncture previously made in the wall of the aorta 12 .
  • Each of the outflow cannulae 110 is preferably composed of a rigid tapered body 122 to facilitate insertion thereof within the open end of the severed intercostal artery 14 .
  • Each of the outflow cannulae 110 includes a balloon occluder 124 located proximal to the outlets 116 to prevent leakage of the blood from the open end of the severed intercostal artery 14 when the outflow cannula 110 is disposed therein and blood is flowed out the outlet 116 .
  • the elongate tubing 102 includes an inflation port 126 , which is in fluid communication with the cavities of the respective balloon occluders 124 via an inflation lumen (not shown). Conveyance of inflation medium into and out of the inflation port 126 effects alternate inflation and deflation of the balloon occluders 124 .
  • each of the balloon occluders 124 can be deflated to facilitate the insertion and removal of the respective outflow cannula 110 into and out of the open end of the severed intercostal artery 14 , and inflated to sealingly secure the respective outflow cannula 110 within the open end of the severed intercostal artery 14 .
  • the inflation port 126 is in fluid communication with the plurality of balloon occluders 124 via a plurality of respective inflation lumens (not shown).
  • the branched multiple vessel perfusion assembly 100 further includes a drug deliver port 127 to allow a physician to introduce drugs, such as, e.g., a neuroprotective agent, into the oxygenated blood.
  • the branched multiple vessel perfusion assembly 100 includes a control mechanism 128 placed within the path of the common portion 104 of the branched conduit 102 .
  • the control mechanism comprises a pump 130 , typically a peristaltic pump, and a cooler 132 . Operation of the pump 130 facilitates and controls the flow of blood through the branched conduit 102 , while operation of the cooler 132 cools the blood, thereby cooling and further protecting the spinal tissue.
  • the control mechanism 128 further includes a thermostat 134 downstream from the cooler 132 , thereby ensuring that the desired temperature of the cooled blood is achieved.
  • the branched multiple vessel perfusion assembly 100 also further include manometers 136 and 138 respectively downstream and upstream from the pump 130 , thereby ensuring that the desired blood pressure within the aorta 12 and the severed intercostal arteries 14 is achieved.
  • the thermostat 134 and manometers 136 and 138 directly provide feedback to the cooler 132 and pump 130 , thereby facilitating automatic control of the blood temperature and respective blood pressures within the aorta 12 and severed intercostal arteries 14 .
  • the blood pressure within the intercostal arteries 14 are maintained above 60 mm, at least for normalthermia.
  • the physician can read the thermostat 134 and manometers 136 and 138 , allowing the physician to manually control the pump 130 and cooler 132 .
  • a manometer 139 can be located on each outflow cannula 116 to provide a direct measurement of the blood pressure in each of the severed intercostal arteries 14 .
  • insertion of the inflow cannula 108 into the aorta upstream from the severed intercostal arteries 14 insertion of the outflow cannulae 116 into the respective severed intercostal arteries 14 , and subsequent operation of the inflation device and control mechanism 128 provides a controlled flow of cooled and oxygenated blood into the spinal arteries 16 via the severed intercostal arteries 14 .
  • inflow cannula 108 can be foregone, in which case, a medium such as, e.g., saline solution, can be flowed from an exterior source into the common portion 104 of the branched conduit 112 .
  • a medium such as, e.g., saline solution
  • the branched multiple vessel perfusion assembly 100 has particular applications in the perfusion of oxygenated blood from the aorta 12 into the open ends of severed intercostal arteries 14 , it can also be employed in other applications requiring the perfusion of oxygenated blood from any large artery to a plurality of open ended vessels without straying from the principles taught by this invention.
  • the chambered multiple vessel perfusion assembly 100 can be used to shunt blood from the aorta 12 to the open ends of severed intercostal arteries 14 .
  • the chambered multiple vessel perfusion assembly 100 generally includes a blood flow conduit 202 , an inflow cannula 204 formed at one end of the blood flow conduit 202 , and a perfusion chamber 206 formed at the other end of the blood flow conduit 202 .
  • the inflow cannula 204 includes a blood flow inlet 208
  • the perfusion chamber 206 includes a substantially enclosed cavity 210 (shown in phantom), such that blood entering the blood flow inlet 208 flows through the blood flow conduit 202 and into the cavity 210 .
  • the perfusion chamber 206 includes a plurality of vessel engaging outlets 212 (shown in phantom) configured to receive the open ends of intercostal arteries 14 to place the lumens of the intercostal arteries 14 in fluid communication with the substantially enclosed cavity 210 .
  • the blood flow conduit 202 is formed of elastomeric tubing.
  • the inflow cannula 204 is constructed in a manner similar to the inflow cannula 108 described above.
  • the perfusion chamber 206 includes a pair of opposing structures 214 , each having an open cavity 216 .
  • the perfusion chamber 206 further includes a hinge 218 on which the opposing structures 214 are mounted, such that the perfusion chamber 206 can be alternately placed into a closed position ( FIG. 5 ) and an open position ( FIG. 6 ).
  • Each of the opposing structures 214 includes a plurality of matching notches 219 formed on an edge 220 opposite the hinge 218 .
  • One of the opposing structures 214 includes an inlet port 222 , which is in communication with the substantially enclosed cavity 210 and is configured to be coupled to the end of the conduit 202 .
  • the open cavities 216 and matching notches 219 of the opposing structures 214 respectively form the cavity 210 and plurality of vessel engaging outlets 212 when the perfusion chamber 206 is in the closed position.
  • the vessel engaging outlets 212 are sized to sealingly engage the open ends of the intercostal arteries 14 , such that blood enters the lumens of the intercostal arteries 14 when the open ends of the intercostal arteries 14 are disposed within the vessel engaging outlets 212 .
  • the spacing between the vessel engaging outlets 212 are preferably equal to the spacing between the integrated plurality of intercostal arteries 14 to facilitate the engagement thereof.
  • the chambered multiple vessel perfusion assembly 100 includes a control mechanism 224 , which includes a pump 226 , cooler 228 , thermostat 230 and manometers 232 and 234 , placed within the path of the conduit 202 .
  • the single vessel perfusion assembly 300 can be used to shunt blood from the aorta 12 to the open end of a severed intercostal artery 14 .
  • the single vessel perfusion assembly 300 generally includes a conduit 302 , an inflow cannula 304 formed at one end of the conduit 302 , and an outflow cannula 306 at the other end of the conduit 302 .
  • the conduit 302 includes a blood lumen 308 extending therethrough.
  • the inflow cannula 304 includes an inlet 310
  • the outflow cannula 306 includes an outlet 312 .
  • the inlet 310 and outlet 312 are in fluid communication with the blood lumen 308 , such that blood entering the inlet 310 flows through the blood lumen 308 and exits the outlet 312 .
  • the conduit 302 is formed of elastomeric tubing.
  • the inflow cannula 304 and outflow cannula 306 are constructed similarly to the respective inflow cannula 108 and outflow cannulae 110 described above.
  • the outflow cannula 306 includes a balloon occluder 314 , and the conduit 302 includes an inflation port 316 , which is in fluid communication with the cavities of the balloon occluders 314 via an inflation lumen (not shown).
  • the single vessel perfusion assembly 300 further includes a drug deliver port 318 to allow a physician to introduce drugs, such as, e.g., a neuroprotective agent, into the oxygenated blood.
  • the single vessel perfusion assembly 300 includes a control mechanism 320 , which includes a pump 322 , cooler 324 , thermostat 326 and manometers 328 and 330 , placed within the path of the conduit 302 .
  • a manometer 332 can be placed at the distal end of the outflow cannula 306 , much like the manometers 139 described above.
  • aortic grafting procedure involves occluding the blood flow within the aorta 12 upstream and downstream from the damaged region, by suitable means, such as, e.g., a clamp 20 .
  • suitable means such as, e.g., a clamp 20 .
  • the intercostal arteries 14 leading to the damaged region of the aorta 12 are then individually severed from the aorta 12 .
  • the aorta 12 is then accessed at a location upstream from the occlusion, and then oxygenated blood is flowed from the aortic access location into the open ends of the individually severed intercostal arteries 14 .
  • Perfusion of the individually severed intercostal arteries 14 can be particularly performed by employing the branched multiple vessel perfusion assembly 100 described above.
  • the plurality of outflow cannulae 110 (shown partially in phantom) are respectively inserted within the open ends of the individually severed intercostal arteries 14 , such that the balloon occluders 124 reside in the lumens thereof.
  • only one of the outflow cannulae 110 is inserted into an open end of one of the individually severed intercostal arteries 14 , preferably, the dominant one, i.e., the intercostal artery 14 with the most backbleeding.
  • the inflow cannula 108 (shown partially in phantom) is inserted through the wall of the aorta 12 upstream from the clamp 20 until the blood flow inlet 114 resides within the lumen of the aorta 12 . This can be accomplished either by a direct stick or through a previously made puncture or opening within the aortic wall. Inflation medium is then conveyed through the inflation port 126 to inflate the balloon occluders 124 , thereby sealing the blood flow outlets 116 within the respective intercostal arteries 14 . To further protect the spinal vasculature, a neuroprotective agent can be flowed into the drug delivery port 127 located on the branched conduit 102 .
  • the control device 128 is then operated to control the perfusion of oxygenated blood within the spinal vasculature. That is, the pump 130 controllingly flows oxygenated blood from the aorta 12 into the inflow cannula 108 , through the branched conduit 102 , out the blood flow outlets 116 , and out through the lumens of the individually severed intercostal arteries 14 to the spinal vasculature.
  • the cooler 132 refrigerates the blood as it travels through the branched conduit 102 , thereby oxygenating and cooling the spinal vasculature of the patient.
  • perfusion of vessels with the cooled and oxygenated blood is limited to the severed intercostal arteries 14 to further facilitate selective hypothermia within the spinal vasculature.
  • a preferred hypothermic temperature will be in the range from 4° C. to 35° C., more preferably from 10° C. to 20° C.
  • the actual temperature which is maintained will depend on the temperature and flow rate of the oxygenated blood, with higher flow rates generally requiring less cooling to achieve the target temperature.
  • Useful flow rates for the oxygenated blood will be in the range from 5 ml/minute to 1000 ml/minute, typically from 50 ml/minute to 400 ml/minute at normalthermia, and from 100 ml/minute to 200 ml/minute at hypothermia. It will be appreciated, of course, that the values of temperature and flow rate will be quite interdependent in that particular optimum values might be selected for individual patients.
  • the temperature of the oxygenated blood and the blood pressure with the aorta 12 and intercostal arteries 14 can be controlled via the thermostat 134 and manometers 136 and 138 . It should be noted that blood can be flowed through fewer than all of the individually severed intercostal arteries 14 , in which case, such remaining individually severed intercostal arteries 14 should be clamped to prevent blood loss therefrom during perfusion of the spinal vasculature.
  • the spinal vasculature can be cooled with a medium other than oxygenated blood.
  • a cooled biocompatible liquid such as, e.g., saline solution can be flowed through the branched conduit 102 from an external source, such as, e.g., an intravenous bag (not shown).
  • a cylindrical region of the aorta 12 encompassing the aneurysm or dissection is then removed and the open ends of the aorta 12 are sutured to a graft.
  • Inflation medium is removed from the inflation port 126 to deflate the balloon occluders 124 , and the inflow cannula 108 and outflow cannulae 110 are respectively removed from the aorta 12 and individually severed intercostal arteries 14 .
  • the intercostal arteries 14 are then sutured to the graft, and the clamp 20 is removed from the aorta 12 , restoring normal circulation to the spinal vasculature.
  • selective spinal vasculature perfusion performed in accordance with a preferred method of the present invention is described in the context of another aortic grafting procedure. Instead of severing the intercostal arteries 14 individually from the aorta 12 as described above, however, an aortic patch 18 (shown in phantom) adjacent the damaged region is excised to integrally severe the intercostal arteries 14 from the aorta 12 .
  • the inflow cannula 204 is inserted through the wall of the aorta 12 , much like the inflow cannula 108 described above.
  • the aortic patch 18 is placed within the substantially enclosed cavity 210 of the perfusion chamber 206 and the integrally severed intercostal arteries 14 are engaged within the vessel engaging outlets 212 , with the openings of the integrally severed intercostal arteries 14 being in fluid communication with the substantially enclosed cavity 210 .
  • the perfusion chamber 206 open as depicted in FIG.
  • the integrally severed intercostal arteries 14 are disposed within notches 219 of one of the opposing structures 214 with the aortic patch 18 lying within the open cavity 216 of the opposing structure 214 .
  • the perfusion chamber 206 is then closed to seal the open ends of the integrally severed intercostal arteries 14 within the perfusion chamber 206 .
  • the control device 224 is operated in much the same manner as the control device 128 described above to control the perfusion of blood within the spinal vasculature. That is, the pump 226 controllingly flows oxygenated blood from the aorta 12 into the inflow cannula 204 , through the conduit 202 , into the perfusion chamber 206 and out through the lumens of the integrally severed intercostal arteries 14 to the spinal vasculature. The cooler 224 refrigerates the blood as it travels through the conduit 202 , thereby inducing selective hypothermia within the spinal vasculature.
  • the assemblies 100 and 200 are interchangeable in this respect.
  • the branched multiple vessel perfusion assembly 100 can be employed to perfuse blood within intercostal arteries 14 that have been integrally severed from the aorta 12 .
  • the chambered multiple vessel perfusion assembly 100 can be employed to perfuse blood within intercostal arteries 14 that have been individually severed from the aorta 12 .
  • the single vessel perfusion assembly 300 described above can be particularly useful in perfusing a single intercostal artery 14 .
  • the outflow cannula 306 (shown partially in phantom) is inserted within the open end of a severed intercostal artery 14
  • the inflow cannula 304 (shown partially in phantom) is inserted through the wall of the aorta 12 , much like the outflow cannulae 110 and inflow cannula 108 described above.
  • Inflation medium is then conveyed through the inflation port 316 to inflate the balloon occluder 314 , thereby sealing the blood flow outlet 312 within the intercostal artery 14 .
  • a neuroprotective agent can be flowed into the drug delivery port 318 .
  • the control device 320 is operated in much the same manner as the control device 128 described above to control the perfusion of blood within the spinal vasculature. That is, the pump 322 controllingly flows oxygenated blood from the aorta 12 into the inflow cannula 304 , through the conduit 302 , out the outflow cannula 306 , and out through the lumen of the intercostal artery 14 to the spinal vasculature.
  • the cooler 324 refrigerates the blood as it travels through the conduit 302 , thereby inducing selective hypothermia within the spinal vasculature.
  • the methods of the present invention are not limited by the type of grafting surgery performed, but can be practiced whenever the open ends of intercostal arteries can be accessed.
  • the open ends of unsevered intercostal arteries 14 can be accessed through a slit 22 made within the wall of the aorta ( FIG. 10 ).
  • Such a procedure finds its usefulness in grafting that involves removing a longitudinal section of the aorta 12 rather than a cylindrical section.
  • the open ends of the unsevered intercostal arteries 14 can be directly perfused in much the same manner as that described above with respect to the branched multiple vessel perfusion assembly 100 .
  • the open ends of unsevered intercostal arteries 12 can also be accessed through a puncture 24 made within the wall of the aorta ( FIG. 11 ).
  • clamps 20 can be used to bracket the intercostal arteries 14 to be perfused, and a shunt 26 can be employed to flow a medium, such as oxygenated blood from the aorta 12 , through the puncture 24 within the wall of the aorta 12 , where the medium is dispersed among the bracketed intercostal arteries 14 .

Abstract

Cooled and oxygenated blood is shunted from the proximal aorta into the open ends of intercostal arteries severed during thoracoabdominal aortic surgery to prevent or minimize the effects of spinal ischemia. This cooled perfusion can be accomplished with a variety of perfusion assemblies. For instance, a single vessel perfusion assembly can be employed to shunt the oxygenated blood from the aorta to the lumen of a single intercostal artery. Cooled perfusion can also be performed with a branched multiple vessel perfusion assembly, which includes a branched conduit comprising a common portion and branch portions. In operation, oxygenated blood flows from the aorta into the inflow cannula, through the blood flow conduit, out of the one or more outflow cannula, and into the intercostal arteries.

Description

  • This is a continuation of U.S. application Ser. No. 10/045,421, filed Jan. 11, 2002, now U.S. Pat. No. 6,817,985, which is a continuation of U.S. application Ser. No. 09/282,771, filed Mar. 31, 1999, now U.S. Pat. No. 6,355,010, both of which are incorporated herein by reference in their entirety.
    • FIELD OF THE INVENTION
  • The present invention relates generally to medical methods and devices, and more particularly, to methods and devices for cooling and perfusing the spinal vasculature of a patient during thoracoabdominal aortic surgery.
    • BACKGROUND
  • Approximately 50,000 patients undergo surgical procedures on the aorta each year for the treatment of various conditions, such as aortic aneurysms, occlusional diseases and aortic dissection. An exemplary procedure includes conventional aortic grafting, which involves clamping the aorta upstream from the damaged region to prevent blood loss at the surgical site, excising a cylindrical portion of the aorta encompassing the damaged region, and replacing the removed portion of the aorta with a graft. During this procedure, the intercostal arteries leading to the damaged region of the aorta are individually severed from the aorta.
  • The cessation of blood flow through the aorta causes spinal ischemia in about 10-15% of patients, due to the reduction or cessation of oxygenated blood within the spinal vasculature that would normally be supplied thereto by the intercostal arteries downstream from the clamped portion of the aorta. Because spinal ischemia can quickly lead to irreversible spinal tissue damage, a minimal amount of time is allowed to suture the intercostal arteries onto the graft. Often, when the intercostal arteries are severed from the aorta, none or very few of them are sutured onto the graft due to the time limitations. The aortic clamp is removed after the graft is attached, thereby supplying oxygenated blood to the spinal vasculature via the unsevered intercostal arteries, albeit in a non-robust manner. Spinal neurological damage is directly related to cross-clamp time and the number of severed intercostal arteries.
  • To ease reattachment to the graft, the intercostal arteries are sometimes integrally severed from the aorta, i.e., patches of the posterior wall of the aorta are excised, each of which carries several intercostal arteries. After the aorta has been grafted, the aortic patch can be sutured onto the graft, minimizing the amount of time it takes to connect the intercostal arteries to the aorta. Regardless of whether the intercostal arteries are individually or integrally severed from the aorta, however, there remains danger of causing irreversible damage to the spinal tissue resulting from ischemia.
  • For these reasons, it would be desirable to provide improved methods and assemblies for preventing spinal ischemia during the performance of surgical procedures on the aorta, and allowing more time to restore a robust blood flow within the spinal vasculature.
    • SUMMARY OF THE INVENTION
  • The invention provides single or multiple vessel perfusion assemblies and methods for selectively treating the spinal vasculature of a patient during thoracoabdominal surgery.
  • Methods performed in accordance with the present invention comprise perfusing the spinal vasculature with a medium by flowing a medium into the open ends of one or more intercostal arteries. The intercostal arteries can be accessed by individually or integrally severing the intercostal arteries from the aorta, or alternatively, the intercostal arteries can be accessed through a puncture or slit within the wall of the aorta. Preferably the medium is cooled to induce hypothermia within the spinal vasculature without cooling the rest of the body (selective spinal hypothermia). The cooled medium can be composed of a biocompatible liquid, such as, e.g., a saline solution, that is flowed from an external source and is cooled. Alternatively, the cooled medium can be composed of oxygenated blood that is shunted from an oxygenated blood filled cavity, such as the heart or proximal aorta upstream from the intercostal arteries and cooled. The characteristics of the cooled medium, such as, e.g., the temperature, flow rate and pressure of the medium is preferably controlled to maintain a viable environment for the spinal vasculature. The methods of the present invention can be performed by employing any vessel perfusion assembly, but are preferably performed by flowing a medium into the plurality of intercostal arteries, which can be facilitated by employing single and multiple vessel perfusion assemblies, such as those described herein.
  • Multiple vessel perfusion assemblies constructed in accordance with the present invention provide a means for simultaneously flowing a medium into the open ends of a plurality of vessels. In a first embodiment, the multiple vessel perfusion assembly includes a branched conduit having a common portion, an inflow cannula formed at one end of the common portion and a plurality of outflow cannulae respectively formed at the other end of the common portion. The branched conduit includes a lumen for conveyance of a medium therethrough. The inflow cannula can comprise any tubular member configured to be inserted through the wall of the heart or proximal aorta, and the outflow cannulae can comprise any tubular members configured to be inserted into the open ends of vessels. The inflow cannula includes an inlet, and the outflow cannulae include outlets, which are in fluid communication with the lumen of the branched conduit. In this manner, insertion of the inflow cannula through the heart or aortic wall and respective insertion of the plurality of outflow cannulae into the open ends of the vessels provides flow of oxygenated blood from the heart or aorta into the vessels. The branched multiple vessel perfusion assembly further includes a cooler for cooling the medium as it passes through the lumen of the branched conduit.
  • In a second embodiment, the multiple vessel perfusion assembly includes a conduit, an inflow cannula formed at one end of the conduit, and a perfusion chamber formed at the other end of the conduit. The conduit includes a lumen, and the inflow cannula and perfusion chamber respectively include an inlet and a substantially enclosed cavity, which are in fluid communication with the lumen of the conduit. The perfusion chamber includes vessel engaging outlets, which are configured to securely receive the open ends of a plurality of integrally severed vessels (an aortic patch). In this manner, insertion of the inflow cannula through the heart or proximal aortic wall, and disposition of the open ends of the severed vessels into the vessel engaging outlets provides simultaneous flow of oxygenated blood from the heart or aorta into the vessel inlets contained within the aortic patch.
  • A single vessel perfusion assembly constructed in accordance with the present invention provides a means for flowing a medium into the open end of a vessel. In an embodiment, the single vessel perfusion assembly includes a conduit, an inflow cannula formed at one end of the conduit and an outflow cannula formed at the other end of the conduit. The conduit includes a lumen for conveyance of a medium therethrough. The inflow cannula includes an inlet, and the outflow cannula includes an outlet, which are in fluid communication with the lumen of the conduit. In this manner, insertion of the inflow cannula through the heart or aortic wall and insertion of the outflow cannula into the open end of the vessel provides flow of oxygenated blood from the heart or aorta into the vessel.
  • Alternatively, the above multiple vessel perfusion assemblies can forego the employment of an inflow cannula. In this case, a medium, such as, e.g., a saline solution, can be suitably introduced into the conduit of the multiple vessel perfusion assemblies. Preferably, the multiple vessel perfusion assemblies further include control devices for conditioning the medium to maintain a viable environment for the tissue to which the vessels lead. For instance, a cooler and associated thermostat can be used to cool and control the temperature of the medium. A pump and associated manometers can be used to control the flow rate and pressure of the medium.
  • Other and further objects, features, aspects, and advantages of the present invention will become better understood with the following detailed description of the accompanying drawings.
    • BRIEF DESCRIPTION OF THE DRAWINGS
  • The drawings illustrate both the design and utility of preferred embodiments of the present invention, in which:
  • FIG. 1 illustrates the systemic arterial circulation of a patient relevant to the present invention;
  • FIG. 2 illustrates a first preferred embodiment of a multiple vessel perfusion assembly constructed in accordance with the present invention;
  • FIG. 3 illustrates an alternative embodiment of the inflow cannula employed in the multiple vessel perfusion assembly of FIG. 2;
  • FIG. 4 illustrates a second preferred embodiment of a multiple vessel perfusion assembly constructed in accordance with the present invention;
  • FIG. 5 illustrates a perfusion chamber employed in the multiple vessel perfusion assembly of FIG. 4, which is particularly shown in a closed position;
  • FIG. 6 illustrates a perfusion chamber employed in the multiple vessel perfusion assembly of FIG. 4, which is particularly shown in an open position;
  • FIG. 7 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of individually severed intercostal arteries by employing multiple vessel perfusion assembly of FIG. 2;
  • FIG. 8 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of integrally severed intercostal arteries by employing the multiple vessel perfusion assembly of FIG. 4;
  • FIG. 9 illustrates a preferred method of placing the open ends of a plurality of integrally severed intercostal arteries within the perfusion chamber of FIG. 5;
  • FIG. 10 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of intercostal arteries through a slit in the aorta;
  • FIG. 11 illustrates a preferred method of simultaneously flowing oxygenated blood from the aorta into the open ends of a plurality of intercostal arteries through a puncture in the aorta; and
  • FIG. 12 illustrates a preferred embodiment of a single vessel perfusion assembly constructed in accordance with the present invention.
  • FIG. 13 illustrates an embodiment of a single vessel perfusion assembly for use in the perfusion of a single intercostal artery.
    • DETAILED DESCRIPTION OF THE PREFERRED EMBODIMENTS
  • Referring to FIG. 1, arterial circulation relevant to the methods of the present invention will be briefly described. Oxygenated blood (represented by arrows) from the heart 10 normally flows through the aorta 12 and into a multitude of intercostal arteries 14, which branch off of the aorta 12. The oxygenated blood then flows from the intercostal arteries 14 into the spinal vasculature, i.e., the posterior spinal arteries 16 and the anterior spinal artery 18 (shown partially in phantom), where it is distributed to the spinal tissue. Because the spinal vasculature is common to all of the intercostal arteries 14, oxygenated blood can still be distributed to the entire spinal tissue even if the blood flow within some of the intercostal arteries 14 ceases. Spinal ischemia will result, however, if the number of intercostal arteries 14 through which the blood flow is ceased is too great, which often occurs as a result of thoracoabdominal aortic surgery.
  • Referring to FIG. 2, a branched multiple vessel perfusion assembly 100 constructed in accordance with a preferred embodiment of the present invention is described. The branched multiple vessel perfusion assembly 100 can be used to shunt blood from the aorta 12 to a plurality of severed arteries, such as, e.g., severed intercostal arteries 14. The vessel perfusion assembly 100 generally includes a branched conduit 102 having a common portion 104, an inflow cannula 108 formed at one end of the common portion 104, and a plurality of outflow cannulae 110 respectively formed at the other end of the common portion 104. The inflow cannula 108 is configured to be inserted through the wall of the aorta 12, and each of the outflow cannulae 110 are configured to be inserted into the open end of a severed intercostal artery, 14. The branched conduit 102 includes a blood lumen 112 extending therethrough. The inflow cannula 108 includes an inlet 114, and the each of the outflow cannulae 110 includes an outlet 116. The inlet 114 and outlets 116 are in fluid communication with the blood lumen 112, such that blood entering the inlet 114 flows through the blood lumen 112 and exits the outlets 116.
  • In the illustrated embodiment, the branched conduit 102 is formed of elastomeric tubing. The inflow cannula 108 includes a hollow needle 118 having a sharpened distal tip, such that the inflow cannula 108 can penetrate the wall of the aorta 12. The inlet 114 is located on the hollow needle 118. Alternatively, as shown in FIG. 3, the inflow cannula 108 includes a blunt access tube 120, which can be inserted inside the aorta 12 through a small incision or puncture previously made in the wall of the aorta 12. Each of the outflow cannulae 110 is preferably composed of a rigid tapered body 122 to facilitate insertion thereof within the open end of the severed intercostal artery 14.
  • Each of the outflow cannulae 110 includes a balloon occluder 124 located proximal to the outlets 116 to prevent leakage of the blood from the open end of the severed intercostal artery 14 when the outflow cannula 110 is disposed therein and blood is flowed out the outlet 116. The elongate tubing 102 includes an inflation port 126, which is in fluid communication with the cavities of the respective balloon occluders 124 via an inflation lumen (not shown). Conveyance of inflation medium into and out of the inflation port 126 effects alternate inflation and deflation of the balloon occluders 124. In this manner, each of the balloon occluders 124 can be deflated to facilitate the insertion and removal of the respective outflow cannula 110 into and out of the open end of the severed intercostal artery 14, and inflated to sealingly secure the respective outflow cannula 110 within the open end of the severed intercostal artery 14. In alternative embodiments, the inflation port 126 is in fluid communication with the plurality of balloon occluders 124 via a plurality of respective inflation lumens (not shown). The branched multiple vessel perfusion assembly 100 further includes a drug deliver port 127 to allow a physician to introduce drugs, such as, e.g., a neuroprotective agent, into the oxygenated blood.
  • The branched multiple vessel perfusion assembly 100 includes a control mechanism 128 placed within the path of the common portion 104 of the branched conduit 102. The control mechanism comprises a pump 130, typically a peristaltic pump, and a cooler 132. Operation of the pump 130 facilitates and controls the flow of blood through the branched conduit 102, while operation of the cooler 132 cools the blood, thereby cooling and further protecting the spinal tissue. The control mechanism 128 further includes a thermostat 134 downstream from the cooler 132, thereby ensuring that the desired temperature of the cooled blood is achieved. The branched multiple vessel perfusion assembly 100 also further include manometers 136 and 138 respectively downstream and upstream from the pump 130, thereby ensuring that the desired blood pressure within the aorta 12 and the severed intercostal arteries 14 is achieved. The thermostat 134 and manometers 136 and 138 directly provide feedback to the cooler 132 and pump 130, thereby facilitating automatic control of the blood temperature and respective blood pressures within the aorta 12 and severed intercostal arteries 14. Preferably, the blood pressure within the intercostal arteries 14 are maintained above 60 mm, at least for normalthermia. Alternatively, the physician can read the thermostat 134 and manometers 136 and 138, allowing the physician to manually control the pump 130 and cooler 132. Alternatively, a manometer 139 can be located on each outflow cannula 116 to provide a direct measurement of the blood pressure in each of the severed intercostal arteries 14.
  • As will be described in further detail below, insertion of the inflow cannula 108 into the aorta upstream from the severed intercostal arteries 14, insertion of the outflow cannulae 116 into the respective severed intercostal arteries 14, and subsequent operation of the inflation device and control mechanism 128 provides a controlled flow of cooled and oxygenated blood into the spinal arteries 16 via the severed intercostal arteries 14.
  • In alternative embodiments, employment of the inflow cannula 108 can be foregone, in which case, a medium such as, e.g., saline solution, can be flowed from an exterior source into the common portion 104 of the branched conduit 112.
  • It should be noted that although the branched multiple vessel perfusion assembly 100 has particular applications in the perfusion of oxygenated blood from the aorta 12 into the open ends of severed intercostal arteries 14, it can also be employed in other applications requiring the perfusion of oxygenated blood from any large artery to a plurality of open ended vessels without straying from the principles taught by this invention.
  • Referring to FIG. 4, a chambered multiple vessel perfusion assembly 100 constructed in accordance with a preferred embodiment of the present invention is described. Like the branched multiple vessel perfusion assembly 100, the chambered multiple vessel perfusion assembly 100 can be used to shunt blood from the aorta 12 to the open ends of severed intercostal arteries 14. The chambered multiple vessel perfusion assembly 100 generally includes a blood flow conduit 202, an inflow cannula 204 formed at one end of the blood flow conduit 202, and a perfusion chamber 206 formed at the other end of the blood flow conduit 202. The inflow cannula 204 includes a blood flow inlet 208, and the perfusion chamber 206 includes a substantially enclosed cavity 210 (shown in phantom), such that blood entering the blood flow inlet 208 flows through the blood flow conduit 202 and into the cavity 210. The perfusion chamber 206 includes a plurality of vessel engaging outlets 212 (shown in phantom) configured to receive the open ends of intercostal arteries 14 to place the lumens of the intercostal arteries 14 in fluid communication with the substantially enclosed cavity 210.
  • In the illustrated embodiment, the blood flow conduit 202 is formed of elastomeric tubing. The inflow cannula 204 is constructed in a manner similar to the inflow cannula 108 described above. Referring to FIGS. 5 and 6, the perfusion chamber 206 includes a pair of opposing structures 214, each having an open cavity 216. The perfusion chamber 206 further includes a hinge 218 on which the opposing structures 214 are mounted, such that the perfusion chamber 206 can be alternately placed into a closed position (FIG. 5) and an open position (FIG. 6). Each of the opposing structures 214 includes a plurality of matching notches 219 formed on an edge 220 opposite the hinge 218. One of the opposing structures 214 includes an inlet port 222, which is in communication with the substantially enclosed cavity 210 and is configured to be coupled to the end of the conduit 202.
  • In this manner, the open cavities 216 and matching notches 219 of the opposing structures 214 respectively form the cavity 210 and plurality of vessel engaging outlets 212 when the perfusion chamber 206 is in the closed position. The vessel engaging outlets 212 are sized to sealingly engage the open ends of the intercostal arteries 14, such that blood enters the lumens of the intercostal arteries 14 when the open ends of the intercostal arteries 14 are disposed within the vessel engaging outlets 212. The spacing between the vessel engaging outlets 212 are preferably equal to the spacing between the integrated plurality of intercostal arteries 14 to facilitate the engagement thereof.
  • Like the branched multiple vessel perfusion assembly 100 described above, the chambered multiple vessel perfusion assembly 100 includes a control mechanism 224, which includes a pump 226, cooler 228, thermostat 230 and manometers 232 and 234, placed within the path of the conduit 202.
  • Referring to FIG. 12, a single vessel perfusion assembly 300 constructed in accordance with a preferred embodiment of the present invention is described. The single vessel perfusion assembly 300 can be used to shunt blood from the aorta 12 to the open end of a severed intercostal artery 14. The single vessel perfusion assembly 300 generally includes a conduit 302, an inflow cannula 304 formed at one end of the conduit 302, and an outflow cannula 306 at the other end of the conduit 302. The conduit 302 includes a blood lumen 308 extending therethrough. The inflow cannula 304 includes an inlet 310, and the outflow cannula 306 includes an outlet 312. The inlet 310 and outlet 312 are in fluid communication with the blood lumen 308, such that blood entering the inlet 310 flows through the blood lumen 308 and exits the outlet 312.
  • In the illustrated embodiment, the conduit 302 is formed of elastomeric tubing. The inflow cannula 304 and outflow cannula 306 are constructed similarly to the respective inflow cannula 108 and outflow cannulae 110 described above. The outflow cannula 306 includes a balloon occluder 314, and the conduit 302 includes an inflation port 316, which is in fluid communication with the cavities of the balloon occluders 314 via an inflation lumen (not shown). The single vessel perfusion assembly 300 further includes a drug deliver port 318 to allow a physician to introduce drugs, such as, e.g., a neuroprotective agent, into the oxygenated blood. Like the branched multiple vessel perfusion assembly 100 described above, the single vessel perfusion assembly 300 includes a control mechanism 320, which includes a pump 322, cooler 324, thermostat 326 and manometers 328 and 330, placed within the path of the conduit 302. Alternatively, a manometer 332 can be placed at the distal end of the outflow cannula 306, much like the manometers 139 described above.
  • With reference to FIG. 7, selective spinal vasculature perfusion performed in accordance with a preferred method of the present invention is described in the context of an aortic grafting procedure performed on a patient. The aortic grafting procedure involves occluding the blood flow within the aorta 12 upstream and downstream from the damaged region, by suitable means, such as, e.g., a clamp 20. The intercostal arteries 14 leading to the damaged region of the aorta 12 are then individually severed from the aorta 12. The aorta 12 is then accessed at a location upstream from the occlusion, and then oxygenated blood is flowed from the aortic access location into the open ends of the individually severed intercostal arteries 14.
  • Perfusion of the individually severed intercostal arteries 14 can be particularly performed by employing the branched multiple vessel perfusion assembly 100 described above. The plurality of outflow cannulae 110 (shown partially in phantom) are respectively inserted within the open ends of the individually severed intercostal arteries 14, such that the balloon occluders 124 reside in the lumens thereof. Alternatively, only one of the outflow cannulae 110 is inserted into an open end of one of the individually severed intercostal arteries 14, preferably, the dominant one, i.e., the intercostal artery 14 with the most backbleeding. The inflow cannula 108 (shown partially in phantom) is inserted through the wall of the aorta 12 upstream from the clamp 20 until the blood flow inlet 114 resides within the lumen of the aorta 12. This can be accomplished either by a direct stick or through a previously made puncture or opening within the aortic wall. Inflation medium is then conveyed through the inflation port 126 to inflate the balloon occluders 124, thereby sealing the blood flow outlets 116 within the respective intercostal arteries 14. To further protect the spinal vasculature, a neuroprotective agent can be flowed into the drug delivery port 127 located on the branched conduit 102.
  • The control device 128 is then operated to control the perfusion of oxygenated blood within the spinal vasculature. That is, the pump 130 controllingly flows oxygenated blood from the aorta 12 into the inflow cannula 108, through the branched conduit 102, out the blood flow outlets 116, and out through the lumens of the individually severed intercostal arteries 14 to the spinal vasculature. The cooler 132 refrigerates the blood as it travels through the branched conduit 102, thereby oxygenating and cooling the spinal vasculature of the patient. Preferably, perfusion of vessels with the cooled and oxygenated blood is limited to the severed intercostal arteries 14 to further facilitate selective hypothermia within the spinal vasculature.
  • A preferred hypothermic temperature will be in the range from 4° C. to 35° C., more preferably from 10° C. to 20° C. The actual temperature which is maintained will depend on the temperature and flow rate of the oxygenated blood, with higher flow rates generally requiring less cooling to achieve the target temperature. Useful flow rates for the oxygenated blood will be in the range from 5 ml/minute to 1000 ml/minute, typically from 50 ml/minute to 400 ml/minute at normalthermia, and from 100 ml/minute to 200 ml/minute at hypothermia. It will be appreciated, of course, that the values of temperature and flow rate will be quite interdependent in that particular optimum values might be selected for individual patients. The temperature of the oxygenated blood and the blood pressure with the aorta 12 and intercostal arteries 14, and thus the blood flow rate, can be controlled via the thermostat 134 and manometers 136 and 138. It should be noted that blood can be flowed through fewer than all of the individually severed intercostal arteries 14, in which case, such remaining individually severed intercostal arteries 14 should be clamped to prevent blood loss therefrom during perfusion of the spinal vasculature.
  • Alternatively, the spinal vasculature can be cooled with a medium other than oxygenated blood. For instance, a cooled biocompatible liquid, such as, e.g., saline solution can be flowed through the branched conduit 102 from an external source, such as, e.g., an intravenous bag (not shown).
  • A cylindrical region of the aorta 12 encompassing the aneurysm or dissection is then removed and the open ends of the aorta 12 are sutured to a graft. Inflation medium is removed from the inflation port 126 to deflate the balloon occluders 124, and the inflow cannula 108 and outflow cannulae 110 are respectively removed from the aorta 12 and individually severed intercostal arteries 14. The intercostal arteries 14 are then sutured to the graft, and the clamp 20 is removed from the aorta 12, restoring normal circulation to the spinal vasculature.
  • With reference to FIG. 8, selective spinal vasculature perfusion performed in accordance with a preferred method of the present invention is described in the context of another aortic grafting procedure. Instead of severing the intercostal arteries 14 individually from the aorta 12 as described above, however, an aortic patch 18 (shown in phantom) adjacent the damaged region is excised to integrally severe the intercostal arteries 14 from the aorta 12.
  • Employment of the chambered multiple vessel perfusion assembly 100 described above can be particularly useful in perfusing such integrally severed intercostal arteries 14. In this connection, the inflow cannula 204 is inserted through the wall of the aorta 12, much like the inflow cannula 108 described above. The aortic patch 18 is placed within the substantially enclosed cavity 210 of the perfusion chamber 206 and the integrally severed intercostal arteries 14 are engaged within the vessel engaging outlets 212, with the openings of the integrally severed intercostal arteries 14 being in fluid communication with the substantially enclosed cavity 210. In particular, with the perfusion chamber 206 open as depicted in FIG. 9, the integrally severed intercostal arteries 14 are disposed within notches 219 of one of the opposing structures 214 with the aortic patch 18 lying within the open cavity 216 of the opposing structure 214. The perfusion chamber 206 is then closed to seal the open ends of the integrally severed intercostal arteries 14 within the perfusion chamber 206.
  • The control device 224 is operated in much the same manner as the control device 128 described above to control the perfusion of blood within the spinal vasculature. That is, the pump 226 controllingly flows oxygenated blood from the aorta 12 into the inflow cannula 204, through the conduit 202, into the perfusion chamber 206 and out through the lumens of the integrally severed intercostal arteries 14 to the spinal vasculature. The cooler 224 refrigerates the blood as it travels through the conduit 202, thereby inducing selective hypothermia within the spinal vasculature.
  • It should be noted that although the use of the multiple vessel perfusion assemblies 100 and 200 were respectively described with reference to individually severed intercostal arteries 14 and integrally severed intercostal arteries 14, the assemblies 100 and 200 are interchangeable in this respect. For instance, the branched multiple vessel perfusion assembly 100 can be employed to perfuse blood within intercostal arteries 14 that have been integrally severed from the aorta 12. Likewise, the chambered multiple vessel perfusion assembly 100 can be employed to perfuse blood within intercostal arteries 14 that have been individually severed from the aorta 12.
  • With reference to FIG. 13, employment of the single vessel perfusion assembly 300 described above can be particularly useful in perfusing a single intercostal artery 14. In this connection, the outflow cannula 306 (shown partially in phantom) is inserted within the open end of a severed intercostal artery 14, and the inflow cannula 304 (shown partially in phantom) is inserted through the wall of the aorta 12, much like the outflow cannulae 110 and inflow cannula 108 described above. Inflation medium is then conveyed through the inflation port 316 to inflate the balloon occluder 314, thereby sealing the blood flow outlet 312 within the intercostal artery 14. To further protect the spinal vasculature, a neuroprotective agent can be flowed into the drug delivery port 318.
  • The control device 320 is operated in much the same manner as the control device 128 described above to control the perfusion of blood within the spinal vasculature. That is, the pump 322 controllingly flows oxygenated blood from the aorta 12 into the inflow cannula 304, through the conduit 302, out the outflow cannula 306, and out through the lumen of the intercostal artery 14 to the spinal vasculature. The cooler 324 refrigerates the blood as it travels through the conduit 302, thereby inducing selective hypothermia within the spinal vasculature.
  • It should also be noted that the methods of the present invention are not limited by the type of grafting surgery performed, but can be practiced whenever the open ends of intercostal arteries can be accessed. For instance, the open ends of unsevered intercostal arteries 14 can be accessed through a slit 22 made within the wall of the aorta (FIG. 10). Such a procedure finds its usefulness in grafting that involves removing a longitudinal section of the aorta 12 rather than a cylindrical section. In this case, the open ends of the unsevered intercostal arteries 14 can be directly perfused in much the same manner as that described above with respect to the branched multiple vessel perfusion assembly 100. The open ends of unsevered intercostal arteries 12 can also be accessed through a puncture 24 made within the wall of the aorta (FIG. 11). In this case, clamps 20 can be used to bracket the intercostal arteries 14 to be perfused, and a shunt 26 can be employed to flow a medium, such as oxygenated blood from the aorta 12, through the puncture 24 within the wall of the aorta 12, where the medium is dispersed among the bracketed intercostal arteries 14.
  • While preferred methods and embodiments have been shown and described, it will be apparent to one of ordinary skill in the art that numerous alterations may be made without departing from the spirit or scope of the invention. Therefore, the invention is not to be limited except in accordance with the following claims.

Claims (1)

1. A vessel perfusion assembly, comprising:
a tubular member having a first end adapted to enter a first vessel, a second end, and a lumen therebetween;
a plurality of tubular branches attached to the second end of the tubular member, each tubular branch having a lumen communicating with the lumen of the tubular member and a distal opening adapted to enter a second vessel;
a sealing mechanism disposed about the distal opening of each tubular branch; and
an extracorporeal cooler communicating with the lumen of the tubular member,
wherein, during use, the first end of the tubular member is inserted into the first vessel, the distal end of each tubular branch is inserted into the second vessel and sealed, and blood flows from the first vessel through the lumen of the tubular member.
US10/990,776 1999-03-31 2004-11-16 Intravascular spinal perfusion and cooling for use during aortic surgery Abandoned US20050070838A1 (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
US10/990,776 US20050070838A1 (en) 1999-03-31 2004-11-16 Intravascular spinal perfusion and cooling for use during aortic surgery

Applications Claiming Priority (3)

Application Number Priority Date Filing Date Title
US09/282,771 US6355010B1 (en) 1999-03-31 1999-03-31 Intravascular spinal perfusion and cooling for use during aortic surgery
US10/045,421 US6817985B2 (en) 1999-03-31 2002-01-11 Intravascular spinal perfusion and cooling for use during aortic surgery
US10/990,776 US20050070838A1 (en) 1999-03-31 2004-11-16 Intravascular spinal perfusion and cooling for use during aortic surgery

Related Parent Applications (1)

Application Number Title Priority Date Filing Date
US10/045,421 Continuation US6817985B2 (en) 1999-03-31 2002-01-11 Intravascular spinal perfusion and cooling for use during aortic surgery

Publications (1)

Publication Number Publication Date
US20050070838A1 true US20050070838A1 (en) 2005-03-31

Family

ID=23083060

Family Applications (3)

Application Number Title Priority Date Filing Date
US09/282,771 Expired - Lifetime US6355010B1 (en) 1999-03-31 1999-03-31 Intravascular spinal perfusion and cooling for use during aortic surgery
US10/045,421 Expired - Fee Related US6817985B2 (en) 1999-03-31 2002-01-11 Intravascular spinal perfusion and cooling for use during aortic surgery
US10/990,776 Abandoned US20050070838A1 (en) 1999-03-31 2004-11-16 Intravascular spinal perfusion and cooling for use during aortic surgery

Family Applications Before (2)

Application Number Title Priority Date Filing Date
US09/282,771 Expired - Lifetime US6355010B1 (en) 1999-03-31 1999-03-31 Intravascular spinal perfusion and cooling for use during aortic surgery
US10/045,421 Expired - Fee Related US6817985B2 (en) 1999-03-31 2002-01-11 Intravascular spinal perfusion and cooling for use during aortic surgery

Country Status (2)

Country Link
US (3) US6355010B1 (en)
WO (1) WO2000057938A1 (en)

Families Citing this family (15)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US6743196B2 (en) 1999-03-01 2004-06-01 Coaxia, Inc. Partial aortic occlusion devices and methods for cerebral perfusion augmentation
US6355010B1 (en) * 1999-03-31 2002-03-12 Coaxia, Inc. Intravascular spinal perfusion and cooling for use during aortic surgery
US6830579B2 (en) 2001-05-01 2004-12-14 Coaxia, Inc. Devices and methods for preventing distal embolization using flow reversal and perfusion augmentation within the cerebral vasculature
US20030028137A1 (en) * 2001-05-18 2003-02-06 Levin Bruce H. Novel hypothermic modalities and direct application of protective agents to neural structures or into CSF
US8361091B2 (en) * 2002-08-23 2013-01-29 Organ Recovery Systems, Inc. Cannulas, cannula mount assemblies, and clamping methods using such cannulas and cannula mount assemblies
US6844959B2 (en) 2002-11-26 2005-01-18 Reflectivity, Inc Spatial light modulators with light absorbing areas
US20070078398A1 (en) * 2005-08-27 2007-04-05 Dextradeur Alan J Multi-branched anti-reflux valve
US8828034B2 (en) 2011-04-29 2014-09-09 Lifeline Scientific, Inc. Cannula
US9642625B2 (en) 2011-04-29 2017-05-09 Lifeline Scientific, Inc. Cannula for a donor organ with or without an aortic cuff or patch
US9022978B2 (en) 2011-04-29 2015-05-05 Lifeline Scientific, Inc. Universal sealring cannula
US9668741B2 (en) 2013-08-14 2017-06-06 Zoll Circulation, Inc. Aortic occluder with tensioned balloons
US9931490B2 (en) 2013-12-17 2018-04-03 Zoll Circulation, Incorporated Control system for arterial catheter
US9737693B2 (en) 2013-12-17 2017-08-22 Zoll Circulation, Inc. Control system for arterial catheter
JO3581B1 (en) * 2014-10-29 2020-07-05 Lilly Co Eli Novel Methyl-Piperidine Compounds Useful for Inhibiting Microsomal Prostaglandin E2 Synthase-1
TW201627299A (en) 2014-10-29 2016-08-01 美國禮來大藥廠 Novel carboxylic acid compounds useful for inhibiting microsomal prostaglandin E2 synthase-1

Citations (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3435824A (en) * 1966-10-27 1969-04-01 Herminio Gamponia Surgical apparatus and related process
US3516405A (en) * 1967-06-20 1970-06-23 United Aircraft Corp Aspirator and control therefor
US4712551A (en) * 1986-10-14 1987-12-15 Rayhanabad Simon B Vascular shunt
US4979937A (en) * 1987-12-22 1990-12-25 Khorasani Ahmad R Method and apparatus involving intercostal and lumbar perfusion
US5391142A (en) * 1992-07-29 1995-02-21 Organetics, Ltd. Apparatus and method for the extracorporeal treatment of the blood of a patient having a medical condition
US5746709A (en) * 1996-04-25 1998-05-05 Medtronic, Inc. Intravascular pump and bypass assembly and method for using the same
US5957963A (en) * 1998-01-23 1999-09-28 Del Mar Medical Technologies, Inc. Selective organ hypothermia method and apparatus
US6436087B1 (en) * 1998-02-03 2002-08-20 Salient Interventional Systems, Inc. Methods and systems for treating ischemia
US6530894B1 (en) * 1999-11-16 2003-03-11 Coaxia, Inc. Aortic shunt with spinal perfusion and cooling device
US6555057B1 (en) * 1998-02-25 2003-04-29 Coaxia, Inc. Intravascular methods and apparatus for isolation and selective cooling of the cerebral vasculature during surgical procedures
US6817985B2 (en) * 1999-03-31 2004-11-16 Coaxia, Inc. Intravascular spinal perfusion and cooling for use during aortic surgery

Family Cites Families (3)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3516408A (en) * 1967-09-21 1970-06-23 Vincent L Montanti Arterial bypass
US4398907A (en) * 1981-07-02 1983-08-16 Crais Thomas F Multiple outlet microarterial bridge for digital replantation
US5288290A (en) * 1991-09-25 1994-02-22 Alcon Surgical, Inc. Multi-ported valve assembly

Patent Citations (11)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3435824A (en) * 1966-10-27 1969-04-01 Herminio Gamponia Surgical apparatus and related process
US3516405A (en) * 1967-06-20 1970-06-23 United Aircraft Corp Aspirator and control therefor
US4712551A (en) * 1986-10-14 1987-12-15 Rayhanabad Simon B Vascular shunt
US4979937A (en) * 1987-12-22 1990-12-25 Khorasani Ahmad R Method and apparatus involving intercostal and lumbar perfusion
US5391142A (en) * 1992-07-29 1995-02-21 Organetics, Ltd. Apparatus and method for the extracorporeal treatment of the blood of a patient having a medical condition
US5746709A (en) * 1996-04-25 1998-05-05 Medtronic, Inc. Intravascular pump and bypass assembly and method for using the same
US5957963A (en) * 1998-01-23 1999-09-28 Del Mar Medical Technologies, Inc. Selective organ hypothermia method and apparatus
US6436087B1 (en) * 1998-02-03 2002-08-20 Salient Interventional Systems, Inc. Methods and systems for treating ischemia
US6555057B1 (en) * 1998-02-25 2003-04-29 Coaxia, Inc. Intravascular methods and apparatus for isolation and selective cooling of the cerebral vasculature during surgical procedures
US6817985B2 (en) * 1999-03-31 2004-11-16 Coaxia, Inc. Intravascular spinal perfusion and cooling for use during aortic surgery
US6530894B1 (en) * 1999-11-16 2003-03-11 Coaxia, Inc. Aortic shunt with spinal perfusion and cooling device

Also Published As

Publication number Publication date
US6817985B2 (en) 2004-11-16
WO2000057938A1 (en) 2000-10-05
US6355010B1 (en) 2002-03-12
US20020058900A1 (en) 2002-05-16

Similar Documents

Publication Publication Date Title
US5707358A (en) Dual concentric balloon catheter for retrograde cardioplegia perfusion
US6123725A (en) Single port cardiac support apparatus
US6817985B2 (en) Intravascular spinal perfusion and cooling for use during aortic surgery
US6866647B2 (en) Aortic shunt with spinal perfusion and cooling device
US6217546B1 (en) Catheter system
US5423745A (en) Irregular surface balloon catheters for body passageways and methods of use
JP3683587B2 (en) Catheter apparatus for providing cardiopulmonary pump support during cardiac surgery
EP1076573B1 (en) Circulatory support system for isolated segmental perfusion
US6267747B1 (en) Aortic catheter with porous aortic root balloon and methods for inducing cardioplegic arrest
US6599266B2 (en) Occlusion cannula and methods of use
US6736790B2 (en) Method and system for selective or isolated integrate cerebral perfusion and cooling
JP4681190B2 (en) Device for controlling extravascular bleeding
US6572640B1 (en) Method and apparatus for cardiopulmonary bypass patient temperature control
US7182727B2 (en) Single port cardiac support apparatus
US4701160A (en) Catheter and method for infusing fluid into a patient
JPH06277278A (en) Perfusion cannula and girdle and trocar used for it
EP1687056B1 (en) Trocar for use during endoscopy
US20070156010A1 (en) Single port cardiac support apparatus related applications
JPH06502774A (en) Methods and devices involving intercostal and lumbar irrigation
CN211407437U (en) Perfusion pipeline for multiple organs
AU712328B2 (en) A catheter system and method for providing cardiopulmonary bypass pump support during heart surgery
GB2411842A (en) Balloon obturator for the aorta

Legal Events

Date Code Title Description
STCB Information on status: application discontinuation

Free format text: ABANDONED -- FAILURE TO RESPOND TO AN OFFICE ACTION