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选择性基质金属蛋白酶抑制可提高实验性梗阻结肠的断裂强度并减少吻合口漏。

Selective matrix metalloproteinase inhibition increases breaking strength and reduces anastomotic leakage in experimentally obstructed colon.

作者信息

Krarup Peter-Martin, Eld Mikkel, Jorgensen Lars Nannestad, Hansen Mark Berner, Ågren Magnus S

机构信息

Digestive Disease Center, Bispebjerg Hospital, University of Copenhagen, Copenhagen, Denmark.

Department of Pathology, Aalborg Hospital, Aalborg, Denmark.

出版信息

Int J Colorectal Dis. 2017 Sep;32(9):1277-1284. doi: 10.1007/s00384-017-2857-x. Epub 2017 Jul 17.

Abstract

PURPOSE

Colonic obstruction causes loss of collagen and impairment of anastomotic integrity by matrix metalloproteinases (MMPs). Unexpectedly, pharmacological MMP inhibition increased anastomotic leakage (AL) in obstructed colon possibly due to the non-selective nature of these compounds and the experimental model applied. We therefore studied the effects of selective MMP inhibition on the healing of anastomoses in colon obstructed by a novel laparoscopic technique.

METHODS

Left colon was obstructed in 38 male Sprague-Dawley rats (226-284 g). After 12 h, stenoses were resected and end-to-end anastomoses constructed. Baseline breaking strength was determined in 6 animals on day 0. The remaining 32 rats were randomized to daily treatment with the selective MMP-8, MMP-9, and MMP-12 inhibitor AZD3342 (n = 16) or vehicle (n = 16). On day 3, anastomoses were evaluated for AL and breaking strength. Isolated anastomotic wound tissue was analyzed on total collagen and pepsin-insoluble and pepsin-soluble collagen by hydroxyproline. The soluble collagens were further differentiated into native, measured by Sircol, and fragmented forms.

RESULTS

Baseline breaking strength was maintained with AZD3342 but decreased by 25% (P = 0.023) in the vehicle group. The anastomotic breaking strength of AZD3342-treated rats was 44% higher (P = 0.008) than the vehicle-treated rats. Furthermore, the AL rate was reduced (P = 0.037) with AZD3342 compared with vehicle treatment. AZD3342 treatment influenced neither the total or insoluble collagen concentrations nor the degree of fragmentation of the soluble collagen triple helices.

CONCLUSION

Selective MMP inhibition increased anastomotic breaking strength and reduced AL after resection of colonic obstruction.

摘要

目的

结肠梗阻会导致胶原蛋白流失,并因基质金属蛋白酶(MMPs)而损害吻合口的完整性。出乎意料的是,药物性MMP抑制会增加梗阻结肠的吻合口漏(AL),这可能是由于这些化合物的非选择性性质以及所应用的实验模型所致。因此,我们研究了选择性MMP抑制对采用新型腹腔镜技术造成梗阻的结肠吻合口愈合的影响。

方法

对38只雄性Sprague-Dawley大鼠(226 - 284克)的左结肠进行梗阻。12小时后,切除狭窄段并进行端端吻合。在第0天对6只动物测定基线断裂强度。其余32只大鼠随机分为两组,一组每天用选择性MMP-8、MMP-9和MMP-12抑制剂AZD3342治疗(n = 16),另一组用赋形剂治疗(n = 16)。在第3天,评估吻合口的AL和断裂强度。通过羟脯氨酸分析分离出的吻合口伤口组织中的总胶原蛋白、胃蛋白酶不溶性和胃蛋白酶可溶性胶原蛋白。可溶性胶原蛋白进一步分为通过Sircol测量的天然形式和片段化形式。

结果

AZD3342组维持了基线断裂强度,但赋形剂组下降了25%(P = 0.023)。AZD3342治疗的大鼠的吻合口断裂强度比赋形剂治疗的大鼠高44%(P = 0.008)。此外,与赋形剂治疗相比,AZD3342治疗使AL发生率降低(P = 0.037)。AZD3342治疗既不影响总胶原蛋白或不溶性胶原蛋白浓度,也不影响可溶性胶原蛋白三螺旋的片段化程度。

结论

选择性MMP抑制可提高结肠梗阻切除术后的吻合口断裂强度并降低AL。

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