Botulinum Toxin Enhanced Foker Process for Long Gap Esophageal Atresia.

Journal of pediatric surgery 2024 Vol.59(12) p. 161628

Izadi S, Koo DC, Shieh HF, Chiu MZ, Demehri FR, Mohammed S, Staffa SJ, Smithers J, Zendejas B

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Abstract

[BACKGROUND] The traction-induced esophageal growth (Foker) process for the treatment of long gap esophageal atresia (LGEA) relies on applying progressive tension to the esophagus to induce growth. Due to its anti-fibrotic and muscle-relaxing properties, we hypothesize that Botulinum Toxin A (BTX) can enhance traction-induced esophageal growth.

[METHODS] A retrospective two-center cohort study was conducted on children who underwent a BTX-enhanced Foker process for LGEA repair from 2021 to 2023. BTX (10 units/ml, 2 units/kg, per esophageal pouch) was applied at the time of traction initiation. Time on traction, complications, and anastomotic outcomes were compared against historical controls (Foker process without BTX) from 2014 to 2021.

[RESULTS] Twenty infants (LGEA type A:12, B:4, C:4; 35% reoperative; median [IQR] age 3 [2-5] months), underwent BTX-enhanced Foker process (thoracotomy with external traction: 9; minimally invasive [MIS] multi-staged internal traction: 11). Mean gap lengths were similar between BTX-enhanced external and external traction control patients (mean [SD], 50.6 mm [12.6] vs. 44.5 mm [11.9], p = 0.21). When compared to controls, the BTX-enhanced external traction process was significantly faster (mean [SD], 12.1 [1.6] days vs. 16.6 [13.2] without BTX, p = 0.04) despite similar preoperative gap lengths. There was no difference in time on traction for those undergoing a minimally invasive process. There were no significant differences in complications or anastomotic outcomes in either cohort.

[CONCLUSION] Botulinum toxin may play a role in accelerating the traction-induced esophageal growth process for LGEA repair. Minimizing time on traction can decrease sedation and paralysis burden while on external traction. Further studies are needed to elucidate the effects of BTX on the esophagus.

[LEVEL OF EVIDENCE] Level III.

[TYPE OF STUDY] Retrospective, Two-center, Cohort study.

추출된 의학 개체 (NER)

유형영어 표현한국어 / 풀이UMLS CUI출처등장
시술 botulinum toxin 보툴리눔독소 주사 dict 3
해부 esophagus scispacy 1
합병증 Esophageal Atresia scispacy 1
합병증 esophageal scispacy 1
합병증 LGEA → long gap esophageal atresia scispacy 1
합병증 esophageal pouch scispacy 1
합병증 LGEA type scispacy 1
약물 [BACKGROUND] The scispacy 1
약물 [RESULTS] scispacy 1
약물 [CONCLUSION] Botulinum toxin scispacy 1
약물 [TYPE OF STUDY] scispacy 1
질환 Esophageal Atresia C0014850
Esophageal Atresia
scispacy 1
질환 external and external traction scispacy 1
질환 paralysis C0522224
Paralysed
scispacy 1
질환 LGEA → long gap esophageal atresia scispacy 1
질환 BTX → Botulinum Toxin A scispacy 1
기타 Botulinum Toxin A scispacy 1
기타 children scispacy 1
기타 C:4 scispacy 1
기타 patients scispacy 1
기타 BTX → Botulinum Toxin A scispacy 1

MeSH Terms

Humans; Esophageal Atresia; Retrospective Studies; Infant; Male; Female; Botulinum Toxins, Type A; Traction; Infant, Newborn; Esophagus; Thoracotomy; Postoperative Complications; Treatment Outcome

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