Proximal Internal Carotid Artery Acute Stroke Secondary to Tandem or Local Occlusion Thrombectomy Trial

Purpose

The primary objective is to establish the efficacy of intra-arterial (IA) mechanical thrombectomy (MT) with extracranial proximal carotid artery acute stenting versus non-stenting approaches in patients with acute ischemic stroke (AIS) from intracranial vessel occlusion (IVO) in the anterior circulation and have a proximal carotid occlusive disease (occlusion or severe stenosis).

Condition

  • Acute Ischemic Stroke

Eligibility

Eligible Ages
Between 18 Years and 79 Years
Eligible Sex
All
Accepts Healthy Volunteers
No

Inclusion Criteria

  1. 18 to 79 years of age (before the 80th birthday) 2. Presenting with symptoms consistent with AIS 3. Imaging evidence of an anterior circulation occlusion of the Internal Carotid Artery (ICA) terminus and/or Middle Cerebral Artery Main Stem (MCA M1), or proximal M2 segment AND extra-cranial proximal carotid occlusion / severe stenosis related to atherosclerosis requiring treatment on non-invasive imaging ≥70% 4. NIHSS ≥ 4 5. Ability to randomize and start endovascular therapy within 16 hours of stroke onset 6. Pre-stroke mRS score 0-2 7. Ability to obtain signed informed consent 8. ASPECTS Score ≥7 via non-contrast CT or MRI (DWI) for subjects ≤6 hours from stroke onset OR ASPECTS Score ≥7 + infarct core volume <50 cc quantified by CTP (rCBF<30%) OR <25 cc quantified by MRI-DWI (AxBxC/2) for subjects with endovascular therapy starting between >6h to 16 hours from stroke onset, given the need for antiplatelet therapy. 9. Acute Neurological Deficit with Imaging evidence of Tandem Lesion: Extracranial carotid occlusion (70% to 100% Using NACET criteria) With or without intracranial vascular occlusion 10. Must be ineligible for IV t-PA therapy or have failed IV t-PA therapy

Exclusion Criteria

  1. Females who are pregnant, or those of child-bearing potential with positive urine or serum beta Human Chorionic Gonadotropin (HCG) test 2. Known severe allergy (more than a rash) to contrast media uncontrolled by medications 3. Refractory hypertension (defined as persistent systolic blood pressure >185 mmHg or diastolic blood pressure >110 mmHg) despite medication 4. CT evidence of the following conditions: - Midline shift or herniation - Evidence of intracranial hemorrhage - Mass effect with effacement of the ventricles 5. Acute bilateral strokes 6. Contraindication to antiplatelet (Aspirin, Plavix, Ticagrelor, Cangrelor), or thrombolytic therapy, or contrast agents. 7. Intracranial tumors other than small meningioma that does not require surgery for one year post randomization 8. Known hemorrhagic diathesis, coagulation factor deficiency, or on anticoagulant therapy with an International Normalized Ratio (INR) of >1.7 or Partial Thromboplastin Time (PTT) > 3 times of normal 9. Baseline platelet count <100,000 per microliter (μl) 10. Life expectancy less than one year prior to stroke onset 11. Participation in another randomized clinical trial that could confound the evaluation of the study outcomes 12. Any other condition (in the opinion of the site investigator) that precludes an endovascular procedure or poses a significant hazard to the patient if an endovascular procedure was performed 13. Proximal carotid stenosis secondary to dissection or vasculitis (.e.g. Takayasu's Arteritis)

Study Design

Phase
Phase 3
Study Type
Interventional
Allocation
Randomized
Intervention Model
Parallel Assignment
Intervention Model Description
Independent Investigator-initiated, designed and conducted non-industry study. A prospective, phase III, randomized, open-label, blinded-endpoint controlled trial (PROBE Design).
Primary Purpose
Treatment
Masking
Single (Outcomes Assessor)

Arm Groups

ArmDescriptionAssigned Intervention
Experimental
MT+CAT 		Non-stenting group constitutes best medical management (BMM)+intra-arterial treatment (IAT) with mechanical thrombectomy (for IVO) added to extra-cranial proximal carotid occlusion angioplasty or aspiration (MT+CAT)
  • Procedure: MT+CAT with PO-AP
    Mechanical Thrombectomy is a treatment for stroke that removes clots that block large blood vessels. Carotid stenting is a procedure that is deployed within the lumen of the carotid artery which treats the narrowing of the carotid artery. With added oral antiplatelet therapy
    Other names:
    • Thrombectomy
Experimental
MT+CAS 		Acute carotid stenting (ACS) approach constitutes BMM+IAT with acute carotid stenting (ACS) of the extracranial proximal carotid artery, spanning the cervical internal carotid artery (ICA), ICA origin, and the distal common carotid artery (CCA, across the bifurcation) as in the example of left (L) carotid stenting figure below (MT+CAS). Within the stenting arm, there will be 2 different subgroups based on the antiplatelet treatment protocol per the site standard of care (oral antiplatelet or IV antiplatelet medication (e.g., Cangrelor or others).
  • Procedure: MT+CAS with IV-AP
    Mechanical Thrombectomy is a treatment for stroke that removes clots that block large blood vessels. Carotid stenting is a procedure that is deployed within the lumen of the carotid artery which treats the narrowing of the carotid artery. With added intravenous antiplatelet therapy.
    Other names:
    • Thrombectomy
  • Procedure: MT+CAS with PO-AP
    Mechanical Thrombectomy is a treatment for stroke that removes clots that block large blood vessels. Carotid stenting is a procedure that is deployed within the lumen of the carotid artery which treats the narrowing of the carotid artery. With added oral antiplatelet therapy.
    Other names:
    • Thrombectomy

Recruiting Locations

Mobile Infirmary Medical Center
Mobile, Alabama 36607
Contact:
Wendy Blount, RN, MSN
wendy.blount@infirmaryhealth.org

Glendale Adventist Medical Center
Glendale, California 91206
Contact:
Lily Villalobos
818-409-8590
villall3@ah.org

University of California, Irvine
Irvine, California 92697
Contact:
Madeline Pak
mspak@hs.uci.edu

Pomona Valley
Pomona, California 91767
Contact:
Raquel Rulloda
raquel.rulloda@pvhmc.org

California Pacific Medical Center/Mils Peninsula Medical Center
San Francisco, California 94107
Contact:
Jalyn Vickroy
jalyn.vickroy@sutterhealth.org

Boca Raton - Baptist Health
Boca Raton, Florida 33486
Contact:
Margaret Scott, RN
561-955-5784
mscott@baptisthealth.net

Delray Medical Center
Delray Beach, Florida 33484
Contact:
Paola Ramirez
paola1.Ramirez@tenethealth.com

Baptist Health Research Institute
Jacksonville, Florida 32207
Contact:
Montserrat Lara Velazquez
904-202-7089
Montserrat.LaraPetrick@bmcjax.com

University of Florida Health Jacksonville
Jacksonville, Florida 32209
Contact:
Yasmeen Shabbir
(904) 244-9856
yasmeen.shabbir@ufhealth.org

University of Miami School of Medicine
Miami, Florida 33136
Contact:
Milagros Castillo
786-450-8145
mcc2407@miami.edu

Orlando Health, Inc.
Orlando, Florida 32806
Contact:
Charlene Carlo
charlene.carlo@orlandohealth.com

University of South Florida
Tampa, Florida 33606
Contact:
Ann Grove
agove@tgh.org

St. Mary's Medical Center
West Palm Beach, Florida 33407
Contact:
Ranjit Singh
909-214-5312
ranjit.singh@tenethealth.com

Piedmont Healthcare
Atlanta, Georgia 30309
Contact:
Shardae Shavers
404-350-2404
shardae.shavers@piedmont.org

WellStar Health System, Inc
Marietta, Georgia 30062
Contact:
Brandon Pickens
brandon.pickens@wellstar.org

Ascension/Alexian Brothers Health System
Chicago, Illinois 60606
Contact:
Diana Sullivan
diana.sullivan@ascension.org

University of Chicago
Chicago, Illinois 60637
Contact:
Ahmad Chahine
ahmad.chahine@bsd.uchicago.edu

Northwestern Medicine Central DuPage Hospital
Winfield, Illinois 60190
Contact:
Rosemarie Baligod
630-933-2113
rosemarie.baligod@nm.org

Indiana University Health Methodist Hospital
Indianapolis, Indiana 46202
Contact:
Terri Strickland
317-948-5450
tstrickland@iuhealth.org

Munster Community Hospital
Munster, Indiana 46321
Contact:
Swayamprava Panda, MS, MPhil
swayamprava.panda@comhs.org

University of Kansas Medical Center
Kansas City, Kansas 66160
Contact:
Margaret Houghton
913-588-5000
mhoughton3@kumc.edu

Baptist Healthcare Systems, Inc
Lexington, Kentucky 40299
Contact:
Melissa Barnes
melissa.barnes@bhsi.com

Ochsner Medical Center
New Orleans, Louisiana 70121
Contact:
William Armstrong, M.S
337-571-0160
william.armstrong@ochsner.org

Louisiana State University Health Sciences Center at Shreveport
Shreveport, Louisiana 71103
Contact:
Tracy Norwood
tracy.norwood@lsuhs.edu

Boston Medical Center
Boston, Massachusetts 02118
Contact:
Robert Contreras
robert.araujocontreras@bmc.org

University of Massachusetts
Worcester, Massachusetts 01655
Contact:
Noelle Bodkin
noelle.bodkin@umassmed.edu

McLaren Flint
Flint, Michigan 48532
Contact:
Kiona Graham
kiona.graham@mclaren.org

Bronson Methodist Hospital/Western Michigan University Homer Stryker M.D. School of Medicine
Kalamazoo, Michigan 49007
Contact:
Lynn Perez
lynn.perez@wmed.edu

Michigan State University
Lansing, Michigan 48912
Contact:
Andrea Zielinksi
Andrea.zielinski@sparrow.org

McLaren Macomb
Mount Clemens, Michigan 48043
Contact:
Valentyna Onishchuk
valentyna.onishchuk@mclaren.org

SSM Health DePaul Hospital
St Louis, Missouri 63044
Contact:
Bridget Gatscher, RN
bridget.gatscher@ssmhealth.com

JFK University Medical Center
Edison, New Jersey 08837
Contact:
Alexandra Burbelo
732-321-7010
alexandra.burbelo@hmhn.org

Rutgers, The State University
Piscataway, New Jersey 08854
Contact:
Roxanne Nagurka
nagurkrm@njms.rutgers.edu

Albany Medical College
Albany, New York 12208
Contact:
Wendy Stewart
stewarw@amc.edu

Northwell Health- South Shore University Hospital
Bay Shore, New York 11706
Contact:
Bryan Klein
bklein3@northwell.edu

Mount Sinai Hospital
New York, New York 10029
Contact:
Emily Svendsen
212-241-3457
emily.svendsen@mountsinai.org

Wake Forest University Health Sciences
Winston-Salem, North Carolina 27157
Contact:
Wendy Jenkins, RN
wejenkin@wakehealth.edu

OhioHealth Research Institute
Columbus, Ohio 43214
Contact:
Wacharaphon Vongchucherd
614-533-5500
wacharaphon.vongchucherd@ohiohealth.com

Mercy Health St. Vincent Medical Center
Toledo, Ohio 43608
Contact:
Kerry Gembreska, RN
kgembreska@mercy.com

University of Oklahoma Health Sciences Center
Oklahoma City, Oklahoma 73104
Contact:
Michael Omini
405-271-4912
michael-omini@ouhsc.edu

Allegheny Health Network Research Institute
Pittsburgh, Pennsylvania 15212
Contact:
Miranda Miller
412-359-8850
miranda.miller@ahn.org

WellSpan Health
York, Pennsylvania 17403
Contact:
Cathy Spahr
cspahr@wellspan.org

Medical University of South Carolina
Charleston, South Carolina 29425
Contact:
Todd LeMatty
lematty@musc.edu

Semmes-Murphey Foundation
Memphis, Tennessee 38120
Contact:
Lorrie Garcia
lgarcia@semmes-murphey.com

HCA Houston Kingwood
Houston, Texas 77004
Contact:
Kelechi Ibezim
kelechi.ibezim@hcahealthcare.com

University of Utah
Salt Lake City, Utah 84112
Contact:
Andrew Grandemange, MBA
andrew.grandemange@hsc.utah.edu

Valley Medical Center
Renton, Washington 98055
Contact:
Dione Froman
dione_froman@valleymed.org

West Virginia Univeristy
Morgantown, West Virginia 26506
Contact:
Jennifer Domico, RN
jennifer.domico@wvumedicine.org

More Details

NCT ID
NCT05611242
Status
Recruiting
Sponsor
Mercy Health Ohio

Study Contact

Jasmine M Olvany, PhD
(419)-251-4264
jolvany@mercy.com

Detailed Description

Independent Investigator-initiated, designed and conducted non-industry study. A prospective, phase III, randomized, open-label, blinded-endpoint controlled trial (PROBE Design). Patients presenting with symptoms of AIS in the anterior circulation with proximal carotid occlusion or severe stenosis will be assigned to either: ARM1 (Control): Non-stenting group constitutes best medical management (BMM)+intra-arterial treatment (IAT) with mechanical thrombectomy (for IVO) added to extra-cranial proximal carotid occlusion treatment with non-stenting approach (MT+CAT) VERSUS ARM2 (Intervention): Acute carotid stenting (ACS) approach constitutes BMM+IAT with acute carotid stenting (ACS) of the extracranial proximal carotid artery, spanning the cervical internal carotid artery (ICA), ICA origin, and the distal common carotid artery (CCA, across the bifurcation) as in the example of left (L) carotid stenting figure below (MT+CAS) Randomization will be 1:1 Mechanical thrombectomy and proximal angioplasty or stenting will be performed with an FDA-cleared devices in accordance with the instructions for use (IFU). The order of each procedure (revascularization of the proximal extra-cranial carotid lesion first or after the intracranial lesion) will be left at discretion of the treating proceduralist. Each treated patient will be followed and assessed for the primary outcome at 3 months and one year after randomization by an independent adjudicator not involved in the procedure. Optional utilization of remote assessment of NIHSS, mRS scale may be provided to selected site

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