有机锡是骨髓间充质基质细胞中过氧化物酶体增殖物激活受体γ和脂肪细胞分化的有效激活剂。

Organotins are potent activators of PPARγ and adipocyte differentiation in bone marrow multipotent mesenchymal stromal cells.

机构信息

Department of Environmental Health, Boston University School of Medicine, Boston, Massachusetts 02118, USA.

出版信息

Toxicol Sci. 2011 Aug;122(2):476-88. doi: 10.1093/toxsci/kfr140. Epub 2011 May 27.

DOI:10.1093/toxsci/kfr140

PMID:21622945

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3155090/

Abstract

Adipocyte differentiation in bone marrow is potentially deleterious to both bone integrity and lymphopoiesis. Here, we examine the hypothesis that organotins, common environmental contaminants that are dual ligands for peroxisome proliferator-activated receptor (PPAR) γ and its heterodimerization partner retinoid X receptor (RXR), are potent activators of bone marrow adipogenesis. A C57Bl/6-derived bone marrow multipotent mesenchymal stromal cell (MSC) line, BMS2, was treated with rosiglitazone, a PPARγ agonist, bexarotene, an RXR agonist, or a series of organotins. Rosiglitazone and bexarotene potently activated adipocyte differentiation; however, bexarotene had a maximal efficacy of only 20% of that induced by rosiglitazone. Organotins (tributyltin [TBT], triphenyltin, and dibutyltin) also stimulated adipocyte differentiation (EC₅₀ of 10-20 nM) but with submaximal, structure-dependent efficacy. In coexposures, both bexarotene and TBT enhanced rosiglitazone-induced adipogenesis. To investigate the contribution of PPARγ to TBT-induced adipogenesis, we examined expression of PPARγ2, as well as its transcriptional target FABP4. TBT-induced PPARγ2 and FABP4 protein expression with an efficacy intermediate between rosiglitazone and bexarotene, similar to lipid accumulation. A PPARγ antagonist and PPARγ-specific small hairpin RNA suppressed TBT-induced differentiation, although to a lesser extent than rosiglitazone-induced differentiation, suggesting that TBT may engage alternate pathways. TBT and bexarotene, but not rosiglitazone, also induced the expression of TGM2 (an RXR target) and ABCA1 (a liver X receptor target). The results show that an environmental contaminant, acting with the same potency as a therapeutic drug, induces PPARγ-dependent adipocyte differentiation in bone marrow MSCs. Activation of multiple nuclear receptor pathways by organotins may have significant implications for bone physiology.

摘要

脂肪细胞在骨髓中的分化对骨完整性和淋巴生成都是有害的。在这里，我们检验了这样一个假设，即有机锡，一种常见的环境污染物，是过氧化物酶体增殖物激活受体（PPAR）γ及其异二聚体伙伴视黄酸 X 受体（RXR）的双重配体，是骨髓脂肪生成的有效激活剂。使用 C57Bl/6 衍生的骨髓多能间充质基质细胞（MSC）系 BMS2 处理罗格列酮，一种 PPARγ激动剂，贝沙罗汀，一种 RXR 激动剂，或一系列有机锡。罗格列酮和贝沙罗汀强烈激活脂肪细胞分化；然而，贝沙罗汀的最大功效只有罗格列酮的 20%。有机锡（三丁基锡[TBT]、三苯基锡和二丁基锡）也刺激脂肪细胞分化（EC₅₀为 10-20 nM），但效果是亚最大的，结构依赖性的。在共暴露中，贝沙罗汀和 TBT 均增强了罗格列酮诱导的脂肪生成。为了研究 PPARγ 对 TBT 诱导的脂肪生成的贡献，我们研究了 PPARγ2 的表达及其转录靶标 FABP4。TBT 诱导 PPARγ2 和 FABP4 蛋白表达的功效介于罗格列酮和贝沙罗汀之间，类似于脂质积累。PPARγ 拮抗剂和 PPARγ 特异性短发夹 RNA 抑制了 TBT 诱导的分化，尽管程度低于罗格列酮诱导的分化，这表明 TBT 可能涉及替代途径。TBT 和贝沙罗汀，但不是罗格列酮，也诱导了 TGM2（RXR 靶标）和 ABCA1（肝 X 受体靶标）的表达。结果表明，一种环境污染物以与治疗药物相同的效力，诱导骨髓 MSC 中 PPARγ 依赖性脂肪细胞分化。有机锡激活多种核受体途径可能对骨生理学有重大影响。

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