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肉毒杆菌毒素 A 和 B 可改善灌注、增加皮瓣存活率、引起血管扩张并预防血栓形成:一项对照动物研究的系统评价和荟萃分析。

Botulinum Toxin A and B Improve Perfusion, Increase Flap Survival, Cause Vasodilation, and Prevent Thrombosis: A Systematic Review and Meta-analysis of Controlled Animal Studies.

机构信息

Bellin Health Systems, Green Bay, WI, USA.

Geisinger Medical Center, Danville, PA, USA.

出版信息

Hand (N Y). 2023 Jan;18(1):22-31. doi: 10.1177/1558944721994250. Epub 2021 Feb 27.

Abstract

BACKGROUND

A systematic review and meta-analysis of case-control animal model studies will help clarify the vascular effects of botulinum toxin (BTX).

METHODS

Preferred Reporting Items of Systematic reviews and Meta-Analyses guidelines were used to identify all animal case-control studies published before September 13, 2020, evaluating the vascular effects of BTX. Primary parameters included the following: perfusion, flap survival, arterial and venous dilation, and arterial and venous thrombosis.

RESULTS

Thirty-six studies with 1032 animals met the systematic review inclusion criteria. Twenty-nine studies had quantifiable data for statistical analysis. Statistically significant increases in perfusion with BTX over saline were detected within 1 day and sustained up to 8 weeks. The following represent weighted mean data from the meta-analysis. The administration of BTX has a 26% increase in both random pattern and pedicled flap survival area over controls. Botulinum toxin causes vasodilation. Botulinum toxin increases vessel diameter in arteries by 40% and in veins by 46% compared with saline controls. The administration of BTX reduces thrombosis by 85% in arteries and by 79% in veins compared with saline controls. Vascular effects were consistent across both BTX-A and BTX-B serotypes, multiple animal species, and various doses. No clear relationships between vascular effects and BTX pretreatment time were identified.

CONCLUSIONS

Perivascular BTX administration intraoperatively or as a chemical delay pretreatment several days before surgery in multiple animal species and models shows multiple changes to the vascular system. Extrapolation of lessons learned from this systematic review and meta-analysis of animal models could expand research and clinical use of BTX in human vascular disease and surgery.

摘要

背景

系统评价和病例对照动物模型研究的荟萃分析将有助于阐明肉毒毒素(BTX)的血管作用。

方法

采用系统评价和荟萃分析的首选报告项目,检索 2020 年 9 月 13 日之前发表的所有评估 BTX 血管作用的动物病例对照研究。主要参数包括:灌注、皮瓣存活率、动脉和静脉扩张以及动脉和静脉血栓形成。

结果

36 项研究共 1032 只动物符合系统评价纳入标准。29 项研究有可用于统计分析的定量数据。在 1 天内检测到 BTX 较盐水显著增加灌注,并持续至 8 周。以下是荟萃分析的加权平均值数据。BTX 给药使随机模式和带蒂皮瓣的存活率比对照增加 26%。肉毒毒素引起血管扩张。与盐水对照相比,BTX 增加动脉血管直径 40%,增加静脉血管直径 46%。BTX 给药使动脉和静脉血栓形成减少 85%和 79%,与盐水对照相比。血管作用在 BTX-A 和 BTX-B 血清型、多种动物物种和不同剂量之间均一致。未发现血管作用与 BTX 预处理时间之间存在明确的关系。

结论

在多种动物物种和模型中,在手术期间或作为化学延迟预处理,将 BTX 给药到血管周围,可引起血管系统的多种变化。从动物模型的系统评价和荟萃分析中得出的经验教训的推断,可以扩大 BTX 在人类血管疾病和手术中的研究和临床应用。

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