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Twelve-month results from a randomized controlled trial comparing differential target multiplexed spinal cord stimulation and conventional spinal cord stimulation in subjects with chronic refractory axial low back pain not eligible for spine surgery.
White, Thomas; Justiz, Rafael; Almonte, Wilson; Micovic, Velimir; Shah, Binit; Anderson, Eric; Kapural, Leonardo; Cordner, Harold; El-Naggar, Amr; Fishman, Michael; Eshraghi, Yashar; Kim, Philip; Abd-Elsayed, Al; Chakravarthy, Krishnan; Millet, Yoann; Sanapati, Mahendra; Harrison, Nathan; Goff, Brandon; Gupta, Mayank; Grewal, Prabhdeep; Wilkinson, Michael; Bundschu, Richard; Will, Andrew; Satija, Pankaj; Li, Sean; Dulebohn, Scott; Broadnax, John; Gekht, Gennady; Wu, Ken; Falowski, Steven; Park, Wesley; Cedeno, David L; Vallejo, Ricardo.
Affiliation
  • White T; Procura Pain and Spine, Pain Management. 111 Vision Park Blvd #100, Shenandoah, TX 77384.
  • Justiz R; Oklahoma Pain Physicians, Pain Management, 4117 NW 122nd St #C, Oklahoma City, OK 73120.
  • Almonte W; Victoria Pain and Rehabilitation, Pain Management, 6902 Zac Lentz Parkway, Victoria, TX 77904.
  • Micovic V; Pain Management Consultants, Pain Management, 7964 Summerlin Lakes Dr, Fort Myers, FL 33907.
  • Shah B; Carolinas Pain Center, Pain Management, 9735 Kincey Ave STE 100, Huntersville, NC 28078.
  • Anderson E; Advanced Pain Institute of Texas, Pain Management, 500 W Main St Suite 230, Lewisville, TX 75057.
  • Kapural L; Carolinas Pain Institute, Pain Management, 145 Kimel Park Dr #330, Winston-Salem, NC 27103.
  • Cordner H; Florida Pain Management Associates, Pain Management, 13825 U.S. Hwy 1, Sebastian, FL 32958.
  • El-Naggar A; DREZ One, Pain Management, 75 Hail Knob Rd, Somerset, KY 42503.
  • Fishman M; Center for Interventional Pain and Spine, Pain Management, 160 N Pointe Blvd Suite 208, Lancaster, PA 17604.
  • Eshraghi Y; Ochsner Medical Center, Pain Management, 1514 Jefferson Highway, New Orleans, LA 70121.
  • Kim P; Center for Interventional Pain and Spine, Pain Management, 160 N Pointe Blvd Suite 208, Lancaster, PA 17604.
  • Abd-Elsayed A; University of Wisconsin, Pain Management, 102 S Park St 3rd floor, Madison, WI 53715.
  • Chakravarthy K; Coastal Research Institute, Pain Management, 6221 Metropolitan Street, Ste. 201, Carlsbad, CA 92009.
  • Millet Y; VA San Diego Healthcare, Pain Management, 3350 La Jolla Village Drive, San Diego, CA 92161.
  • Sanapati M; Procura Pain and Spine, Pain Management. 111 Vision Park Blvd #100, Shenandoah, TX 77384.
  • Harrison N; Global Scientific Innovations, Pain Management, 1101 Professional Blvd, Ste 208, Evansville, IN 47714.
  • Goff B; Ochsner Medical Center, Pain Management, 1514 Jefferson Highway, New Orleans, LA 70121.
  • Gupta M; Burkhart Research Institute for Orthopaedics, Pain Management, 400 Concord Plaza Dr, San Antonio, TX, 78216.
  • Grewal P; Neuroscience Research Center, Pain Management. 10995 Quivira Road, Overland Park, KS 66210.
  • Wilkinson M; Burkhart Research Institute for Orthopaedics, Pain Management, 400 Concord Plaza Dr, San Antonio, TX, 78216.
  • Bundschu R; Pain Medicine Associates Surgery Center, Pain Management, 101 Med Tech Pkwy #200, Johnson City, TN 37604.
  • Will A; Coastal Orthopedics and Sports Medicine and Pain Management, Pain Management, 6202 17th Ave W, Bradenton, FL 34209.
  • Satija P; Twin Cities Pain Clinic; Pain Management, 7235 Ohms Lane, Edina, MN.
  • Li S; Pain & Headache Centers of Texas, Pain Management, 313 La Concha Lane, Suite 120, Houston, TX 77054.
  • Dulebohn S; National Spine and Pain Premier Pain Centers, Pain Management, 170 Ave at the Cmns Suite 6, Shrewsbury, NJ 07702.
  • Broadnax J; Pain Medicine Associates Surgery Center, Pain Management, 101 Med Tech Pkwy #200, Johnson City, TN 37604.
  • Gekht G; Advanced Pain Institute of Texas, Pain Management, 500 W Main St Suite 230, Lewisville, TX 75057.
  • Wu K; Coastal Orthopedics and Sports Medicine and Pain Management, Pain Management, 6202 17th Ave W, Bradenton, FL 34209.
  • Falowski S; Procura Pain and Spine, Pain Management. 111 Vision Park Blvd #100, Shenandoah, TX 77384.
  • Park W; Center for Interventional Pain and Spine, Pain Management, 160 N Pointe Blvd Suite 208, Lancaster, PA 17604.
  • Cedeno DL; SGX Medical LLC, Clinical Research, 33 Derby Way, Bloomington, IL 61704.
  • Vallejo R; SGX Medical LLC, Clinical Research, 33 Derby Way, Bloomington, IL 61704.
N Am Spine Soc J ; 19: 100528, 2024 Sep.
Article in En | MEDLINE | ID: mdl-39229594
ABSTRACT

Background:

Successful treatments for intractable chronic low back pain (CLBP) in patients who are not eligible for surgical interventions are scarce. The superior efficacy of differential target multiplexed spinal cord stimulation (DTM SCS) to conventional SCS (Conv-SCS) on the treatment of CLBP in patients with persistent spinal pain syndrome (PSPS) who have failed surgical interventions (PSPS-T2) motivated the evaluation of DTM SCS versus Conv-SCS on PSPS patients who are non-surgical candidates (PSPS-T1).

Methods:

This is a prospective, open label, crossover, post-market randomized controlled trial in 20 centers across the United States. Eligible patients were randomized to either DTM SCS or Conv-SCS in a 11 ratio. Primary endpoint was CLBP responder rate (percentage of subjects with ≥50% CLBP relief) at 3-month in randomized subjects who completed trialing (modified intention-to-treat population). Patients were followed up to 12 months. Secondary endpoints included change of CLBP and leg pain, responder rates, changes in disability, quality of life, patient satisfaction and global impression of change, and safety profile. An optional crossover was available at 6-month to all patients.

Results:

About 121 PSPS-T1 subjects with CLBP and leg pain mostly associated with degenerative disc disease and radiculopathy and who were not eligible for spine surgery were randomized. CLBP responder rate with DTM SCS (93.5%) was superior to Conv-SCS (36.4%) at the primary endpoint. Superior CLBP responder rates (88.1%-90.5%) were obtained with DTM SCS at all other timepoints. Mean CLBP reduction with DTM SCS (6.52 cm) was superior to that with Conv-SCS (3.01 cm) at the primary endpoint. Similar CLBP reductions (6.23-6.43 cm) were obtained with DTM SCS at other timepoints. DTM SCS provided significantly better leg pain reduction and responder rate, improvement of disability and quality of life, and better patient satisfaction and global impression of change. 90.9% of Conv-SCS subjects who crossed over were CLBP responders at completion of the study. Similar safety profiles were observed between the two groups.

Conclusion:

DTM SCS for chronic CLBP in nonsurgical candidates is superior to Conv-SCS. Improvements were sustained and provided significant benefits on the management of these patients.
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: N Am Spine Soc J Year: 2024 Document type: Article Country of publication: Estados Unidos
Fulltext
Add to My VHL
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Full text: 1 Collection: 01-internacional Database: MEDLINE Language: En Journal: N Am Spine Soc J Year: 2024 Document type: Article Country of publication: Estados Unidos