Literature DB >> 16860080

An internally covered (lined) self-expanding metal esophageal stent: tissue response in a porcine model.

Todd H Baron1, Lawrence J Burgart, Nicole L Pochron.   

Abstract

BACKGROUND: Self-expandable metal stents (SEMS) palliate malignant dysphagia but may embed in tissue, produce granulation tissue, and prevent removal.
OBJECTIVE: Our purpose was to evaluate in a porcine model the tissue response induced by a new esophageal SEMS completely coated internally rather than externally.
DESIGN: Eight Yucatan pigs were studied. Each animal underwent placement of 2 stents: 1 study stent and 1 control stent. SEMS were placed proximally or distally by random assignment. Follow-up endoscopy was performed 1, 2, 3, and 4 weeks after implantation. Ease of stent removal was assessed at 2 weeks and 4 weeks after placement.
SETTING: Animal laboratory.
INTERVENTIONS: Endoscopic placement of study stents (Alveolus ES-STS, Alveolus, Inc, Charlotte, NC; 18 mm diameter, fully covered internally) and control stents (Ultraflex stent, Boston Scientific, Natick, Mass; microvasive, 18 mm midbody, subtotally covered externally). MAIN OUTCOME MEASUREMENTS: Extent of granulation tissue and stent-induced esophageal injury.
RESULTS: The tissue hyperplasia response of the study stents was endoscopically graded as mild to moderate. All study stents were endoscopically removed easily and atraumatically. Control stents produced severe granulation tissue formation with complete embedding of the uncovered stent ends; endoscopic removal was possible but resulted in trauma and endoscopically visible bleeding. Histopathologic findings revealed minimal tissue response at the ends of the study stents and severe pseudopolyps in the embedded portion of the control stent. Stent migration occurred in 7 of 8 study stents and 4 of 8 control stents. LIMITATIONS: Animal model lacks stricture.
CONCLUSIONS: Fully internally lined SEMS may resist tissue embedding and hyperplasia and may be removable. Human studies are needed to assess applicability to treatment of benign and malignant esophageal disease.

Entities:  

Mesh:

Year:  2006        PMID: 16860080     DOI: 10.1016/j.gie.2006.03.936

Source DB:  PubMed          Journal:  Gastrointest Endosc        ISSN: 0016-5107            Impact factor:   9.427


  10 in total

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Journal:  Dig Dis Sci       Date:  2007-06-28       Impact factor: 3.199

2.  Endoscopic stenting for benign upper gastrointestinal strictures and leaks.

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3.  A novel biodegradable esophageal stent: results from mechanical and animal experiments.

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4.  History of the Use of Esophageal Stent in Management of Dysphagia and Its Improvement Over the Years.

Authors:  Kulwinder S Dua
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5.  Successful rigid endoscopic removal of an esophageal subtotally covered nitinol stent 11 months after initial placement.

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7.  Nanofunctionalized Stent-Mediated Local Heat Treatment for the Suppression of Stent-Induced Tissue Hyperplasia.

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8.  Successful closure of pharyngo-cutaneous and phayryngo-tracheal fistulas using removable hypopharyngeal stent after laryngectomy for laryngeal carcinoma.

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9.  Establishing a rabbit model of malignant esophagostenosis using the endoscopic implantation technique for studies on stent innovation.

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10.  Efficacy of Gastric Balloon Dilatation and/or Retrievable Stent Insertion for Pyloric Spasms after Pylorus-Preserving Gastrectomy: Retrospective Analysis.

Authors:  Jae Seok Bae; Se Hyung Kim; Cheong-Il Shin; Ijin Joo; Jeong Hee Yoon; Hyuk-Joon Lee; Han-Kwang Yang; Jee Hyun Baek; Tae Han Kim; Joon Koo Han; Byung Ihn Choi
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  10 in total

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