Octreotide modulates the effects on fibrosis of TNF-α, TGF-β and PDGF in activated rat hepatic stellate cells

Stefanos Klironomos , George Notas , Ourania Sfakianaki , Foteini Kiagiadaki , Costas Xidakis , Elias Kouroumalis
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引用次数: 20

Abstract

Background and aims

Somatostatin and its analogs may influence hepatic fibrosis interfering through several mechanisms. The aim of this study was to investigate the effect of octreotide on cytokine activated hepatic stellate cells (HSC).

Methods

Primary HSCs were isolated from rats and were cultured on plastic for activation. Expression of somatostatin receptors (SSTR) was investigated in cultured HSCs by immunofluorescence and western blot. The effect of octreotide on cellular proliferation was studied with the MTT assay and western blot for α1-procollagen (α1-PROC) production in TNFα, TGF-β1 or PDGF treated HSCs. Phosphotyrosine (PTP) and phosphoserine–phosphothreonine (STP) phosphatases inhibition was performed with sodium orthovanadate and okadaic acid respectively.

Results

Activated HSC express SSTR subtypes 1, 2A, 2B, 3 and 4 and their expression is enhanced by further HSC activation. Octreotide did not have an effect on HSC proliferation but inhibited plastic induced α1-PROC production. Interestingly, it enhanced PDGF-induced HSC proliferation but inhibited PDGF and TGFβ1 dependent expression of α1-PROC, while an opposite effect was observed in TNFα-induced cell proliferation and collagen production. PTP inhibition reversed the inhibitory effect of octreotide on α1-PROC, but potentiated its effect on PDGF and TGFβ1 dependent α1-PROC production. Finally, STP inhibition profoundly inhibited α1-PROC expression in all cases suggesting that both STP and PTP phosphatases are important regulators of pro-fibrotic mechanisms.

Conclusions

The net effect of octreotide on HSCs and therefore liver fibrosis is subject to the cytokine microenvironment of these cells. This effect is modulated by PTPs and STPs inhibition. Especially in the case of STPs their profibrotic effects could be an interesting new therapeutic target in liver fibrosis.

奥曲肽调节活化大鼠肝星状细胞TNF-α、TGF-β和PDGF的纤维化作用
背景和目的生长抑素及其类似物可能通过多种机制干扰肝纤维化。本研究旨在探讨奥曲肽对细胞因子活化的肝星状细胞(HSC)的影响。方法从大鼠体内分离原代造血干细胞,在塑料上培养活化。采用免疫荧光法和western blot法研究生长抑素受体(SSTR)在培养造血干细胞中的表达。采用MTT法和western blot检测TNFα、TGF-β1和PDGF处理的造血干细胞α1-前胶原(α1-PROC)的生成,研究奥曲肽对造血干细胞增殖的影响。分别用原钒酸钠和冈田酸抑制磷酸酪氨酸(PTP)和磷酸丝氨酸-磷酸苏氨酸(STP)磷酸酶。结果活化后的HSC表达SSTR亚型1、2A、2B、3和4,进一步活化后其表达增强。奥曲肽对HSC增殖无影响,但对塑性诱导的α1-PROC产生有抑制作用。有趣的是,它增强了PDGF诱导的HSC增殖,但抑制了PDGF和TGFβ1依赖性α1-PROC的表达,而在tnf α诱导的细胞增殖和胶原生成中观察到相反的作用。PTP抑制逆转了奥曲肽对α1-PROC的抑制作用,但增强了其对PDGF和TGFβ1依赖性α1-PROC产生的影响。最后,在所有情况下,STP抑制都能显著抑制α1-PROC的表达,这表明STP和PTP磷酸酶都是促纤维化机制的重要调节因子。结论奥曲肽对造血干细胞的净效应取决于造血干细胞的细胞因子微环境。这种效应是由ptp和STPs抑制调节的。特别是在STPs的情况下,它们的促纤维化作用可能是肝纤维化的一个有趣的新治疗靶点。
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来源期刊
Regulatory Peptides
Regulatory Peptides 医学-内分泌学与代谢
自引率
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审稿时长
2 months
期刊介绍: Regulatory Peptides provides a medium for the rapid publication of interdisciplinary studies on the physiology and pathology of peptides of the gut, endocrine and nervous systems which regulate cell or tissue function. Articles emphasizing these objectives may be based on either fundamental or clinical observations obtained through the disciplines of morphology, cytochemistry, biochemistry, physiology, pathology, pharmacology or psychology.
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