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大鼠肾近端小管和远端小管细胞原代培养物对化学诱导毒性的易感性。

Susceptibility of primary cultures of proximal tubular and distal tubular cells from rat kidney to chemically induced toxicity.

作者信息

Lash L H, Tokarz J J, Pegouske D M

机构信息

Department of Pharmacology, Wayne State University School of Medicine, Detroit, MI 48201, USA.

出版信息

Toxicology. 1995 Nov 30;103(2):85-103. doi: 10.1016/0300-483x(95)03110-2.

Abstract

Isolated proximal tubular (PT) and distal tubular (DT) cells from rat kidney were cultured for up to 9 days under serum-free, hormonally-defined conditions on 35-mm polystyrene culture dishes. Several hormonal and growth factor supplements were assessed for their ability to promote growth (increased protein and DNA content) and stability of differentiated phenotype (high activities of gamma-glutamyltransferase and alkaline phosphatase as brush-border membrane markers in PT cells; maintenance of high activities of glutamate dehydrogenase as a mitochondrial marker in both PT and DT cells; maintenance of low and high activities of lactate dehydrogenase in PT and DT cells, respectively; expression of cytokeratins). Basal supplemented media (DMEM/F12, 1:1 v/v) contained insulin, hydrocortisone, epidermal growth factor, sodium selenite and transferrin as supplements. Additionally, triiodothyronine selectively promoted growth and stability of differentiated phenotype in PT cells and thyrocalcitonin selectively promoted growth and stability of differentiated phenotype in DT cells. On Day 3 of primary culture, PT and DT cells were incubated for up to 8 h with either tert-butyl hydroperoxide (tBH; 0.5-10 mM), methyl vinyl ketone (MVK; 1-10 mM), or p-aminophenol (PAP; 1-10 mM) and cellular injury, as assessed by cellular release of lactate dehydrogenase, was determined. DT cells were significantly more susceptible to injury from both tBH and MVK, but the two cell populations were equally susceptible to injury from PAP, which is the same susceptibility pattern seen in freshly isolated cells. These results suggest that primary cultures of rat renal PT and DT cells reflect similar biochemical properties as freshly isolated cells and are, therefore, useful models for study of chemically induced injury.

摘要

从大鼠肾脏分离出的近端肾小管(PT)细胞和远端肾小管(DT)细胞,在无血清、激素限定条件下,于35毫米聚苯乙烯培养皿中培养长达9天。评估了几种激素和生长因子补充剂促进生长(增加蛋白质和DNA含量)以及维持分化表型稳定性(PT细胞中γ-谷氨酰转移酶和碱性磷酸酶作为刷状缘膜标志物的高活性;PT和DT细胞中谷氨酸脱氢酶作为线粒体标志物的高活性维持;PT和DT细胞中乳酸脱氢酶分别维持低活性和高活性;细胞角蛋白的表达)的能力。基础补充培养基(DMEM/F12,1:1 v/v)含有胰岛素、氢化可的松、表皮生长因子、亚硒酸钠和转铁蛋白作为补充剂。此外,三碘甲状腺原氨酸选择性地促进PT细胞的生长和分化表型的稳定性,而降钙素选择性地促进DT细胞的生长和分化表型的稳定性。在原代培养的第3天,PT和DT细胞分别用叔丁基过氧化氢(tBH;0.5 - 10 mM)、甲基乙烯基酮(MVK;1 - 10 mM)或对氨基酚(PAP;1 - 10 mM)孵育长达8小时,并通过乳酸脱氢酶的细胞释放来评估细胞损伤情况。DT细胞对tBH和MVK引起的损伤明显更敏感,但这两种细胞群体对PAP引起的损伤敏感性相同,这与新鲜分离细胞中观察到的敏感性模式相同。这些结果表明,大鼠肾PT和DT细胞的原代培养反映出与新鲜分离细胞相似的生化特性,因此是研究化学诱导损伤的有用模型。

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