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携带脑啡肽的单纯疱疹病毒-1可降低慢性胰腺炎模型中的炎症反应和热板敏感性。

Enkephalin-encoding herpes simplex virus-1 decreases inflammation and hotplate sensitivity in a chronic pancreatitis model.

作者信息

Yang Hong, McNearney Terry A, Chu Rong, Lu Ying, Ren Yong, Yeomans David C, Wilson Steven P, Westlund Karin N

机构信息

Dept of Neuroscience and Cell Biology, University of Texas Medical Branch, Galveston, TX, USA.

出版信息

Mol Pain. 2008 Feb 28;4:8. doi: 10.1186/1744-8069-4-8.

Abstract

BACKGROUND

A chronic pancreatitis model was developed in young male Lewis rats fed a high-fat and alcohol liquid diet beginning at three weeks. The model was used to assess time course and efficacy of a replication defective herpes simplex virus type 1 vector construct delivering human cDNA encoding preproenkephalin (HSV-ENK).

RESULTS

Most surprising was the relative lack of inflammation and tissue disruption after HSV-ENK treatment compared to the histopathology consistent with pancreatitis (inflammatory cell infiltration, edema, acinar cell hypertrophy, fibrosis) present as a result of the high-fat and alcohol diet in controls. The HSV-ENK vector delivered to the pancreatic surface at week 3 reversed pancreatitis-associated hotplate hypersensitive responses for 4-6 weeks, while control virus encoding beta-galactosidase cDNA (HSV-beta-gal) had no effect. Increased Fos expression seen bilaterally in pain processing regions in control animals with pancreatitis was absent in HSV-ENK-treated animals. Increased met-enkephalin staining was evident in pancreas and lower thoracic spinal cord laminae I-II in the HSV-ENK-treated rats.

CONCLUSION

Thus, clear evidence is provided that site specific HSV-mediated transgene delivery of human cDNA encoding preproenkephalin ameliorates pancreatic inflammation and significantly reduces hypersensitive hotplate responses for an extended time consistent with HSV mediated overexpression, without tolerance or evidence of other opiate related side effects.

摘要

背景

从三周龄开始,给年轻雄性Lewis大鼠喂食高脂酒精液体饮食,建立慢性胰腺炎模型。该模型用于评估携带编码前脑啡肽原的人cDNA的复制缺陷型单纯疱疹病毒1型载体构建体(HSV-ENK)的时间进程和疗效。

结果

最令人惊讶的是,与对照组因高脂酒精饮食导致的符合胰腺炎的组织病理学表现(炎症细胞浸润、水肿、腺泡细胞肥大、纤维化)相比,HSV-ENK治疗后炎症和组织破坏相对较少。在第3周递送至胰腺表面的HSV-ENK载体使胰腺炎相关的热板超敏反应逆转4至6周,而编码β-半乳糖苷酶cDNA的对照病毒(HSV-β-gal)则无作用。在接受HSV-ENK治疗的动物中,未出现对照组胰腺炎动物双侧疼痛处理区域中所见的Fos表达增加。在接受HSV-ENK治疗的大鼠中,胰腺和胸段脊髓I-II层中甲硫脑啡肽染色增加明显。

结论

因此,有明确证据表明,位点特异性HSV介导的携带编码前脑啡肽原的人cDNA的转基因递送可改善胰腺炎症,并在与HSV介导的过表达一致的较长时间内显著降低热板超敏反应,且无耐受性或其他阿片类药物相关副作用的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/221e/2292157/29d85bb8c124/1744-8069-4-8-1.jpg

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