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哈洛芬酮抑制胰腺星状细胞激活可预防胰腺异种移植瘤的发展。

Inhibition of pancreatic stellate cell activation by halofuginone prevents pancreatic xenograft tumor development.

机构信息

Institute of Animal Sciences, Volcani Center, Bet Dagan, Israel.

出版信息

Pancreas. 2010 Oct;39(7):1008-15. doi: 10.1097/MPA.0b013e3181da8aa3.

Abstract

OBJECTIVES

Most solid tumors consist of neoplastic and nonneoplastic cells and extracellular matrix components. In the pancreas, activated stellate cells (PSCs) are the source of the extracellular matrix proteins. We evaluated the significance of PSC activation in tumor establishment and development in mouse xenografts.

METHODS

Xenografts were established by implanting human pancreatic cancer cells (MiaPaca-2) subcutaneously or orthotopically by injecting them into the spleen. Fibrosis was induced by cerulein. Collagen level was evaluated by Sirius red staining. Prolyl 4-hydroxylase β and stellate cell activation-associated protein (Cygb/STAP) were determined by immunohistochemistry.

RESULTS

Halofuginone inhibited subcutaneous tumor development implanted with Matrigel and reduced collagen and prolyl 4-hydroxylase β levels. Few tumors, which developed slowly, were observed after MiaPaca-2 implantation without Matrigel. Increase in tumor number and rate of development were observed with addition of PSCs from control pancreas, and further increase was observed when the PSCs were from cerulein-treated mice. Preincubation of the PSCs with halofuginone elicited Cygb/STAP level reduction and tumor growth inhibition. More tumors developed orthotopically in cerulein-treated mice than in controls; this was prevented by halofuginone.

CONCLUSIONS

Extracellular matrix production by activated PSCs is essential for tumor establishment and growth. Thus, inhibition of PSC activation is a viable means of reducing pancreatic tumor development.

摘要

目的

大多数实体瘤由肿瘤细胞和非肿瘤细胞以及细胞外基质成分组成。在胰腺中,活化的星状细胞(PSCs)是细胞外基质蛋白的来源。我们评估了 PSC 在小鼠异种移植中肿瘤形成和发展中的意义。

方法

通过将人胰腺癌细胞(MiaPaca-2)皮下或通过注射到脾脏中建立异种移植物。用 Cerulein 诱导纤维化。通过 Sirius red 染色评估胶原蛋白水平。通过免疫组织化学测定脯氨酰 4-羟化酶β和星状细胞激活相关蛋白(Cygb/STAP)。

结果

Halofuginone 抑制了植入 Matrigel 的皮下肿瘤的发展,并降低了胶原蛋白和脯氨酰 4-羟化酶β的水平。在没有 Matrigel 的情况下植入 MiaPaca-2 后,观察到生长缓慢的少数肿瘤。添加来自对照胰腺的 PSCs 会增加肿瘤数量和发展速度,而添加来自 Cerulein 处理小鼠的 PSCs 则会进一步增加。用 Halofuginone 预先孵育 PSCs 可降低 Cygb/STAP 水平并抑制肿瘤生长。Cerulein 处理的小鼠中比对照组更多的肿瘤发生原位,这可以被 Halofuginone 预防。

结论

活化的 PSCs 产生细胞外基质对于肿瘤的建立和生长是必需的。因此,抑制 PSC 的激活是减少胰腺肿瘤发展的可行方法。

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