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胎盘谷胱甘肽转移酶的纯化、诱导及分布:大鼠化学性肝癌发生过程中一种新的癌前细胞标志物酶

Purification, induction, and distribution of placental glutathione transferase: a new marker enzyme for preneoplastic cells in the rat chemical hepatocarcinogenesis.

作者信息

Satoh K, Kitahara A, Soma Y, Inaba Y, Hatayama I, Sato K

出版信息

Proc Natl Acad Sci U S A. 1985 Jun;82(12):3964-8. doi: 10.1073/pnas.82.12.3964.

Abstract

A polypeptide of Mr 26,000 and pI 6.7 that was markedly increased in rat livers bearing hyperplastic nodules (HNs) induced by chemical carcinogens was identified immunochemically as the subunit of neutral glutathione (GSH) transferase (GSHTase; RX:glutathione R-transferase, EC 2.5.1.18; also called GSH S-transferase) purified from placenta (GSHTase-P) and was demonstrated immunohistochemically to be localized in preneoplastic foci and HNs. In the present study, GSHTase-P has been purified from the HN-bearing liver, and the distribution and inducibility have been examined quantitatively using anti-GSHTase-P antibody. Elevation of GSHTase-P in the HN-bearing livers was also confirmed by in vitro translation of mRNAs isolated from the HN-bearing livers. The purified GSHTase-P was homogeneous in size but had two charge isomers on two-dimensional gel electrophoresis. In normal tissues, including liver, placenta, and fetal liver, the protein content of GSHTase-P was generally low but was significantly high in kidney and pancreas. In contrast, the amount of GSHTase-P in HN-bearing livers (primary hepatomas) and transplantable Morris hepatoma 5123D were several 10-fold higher than that in normal liver but were undetectably low in transplantable Yoshida ascites hepatoma AH 130. Different from ordinary drug-metabolizing enzymes, GSHTase-P was uninducible by administration of drugs and carcinogens prior to appearance of the preneoplastic foci and HNs. In addition, species specificity of GSHTase-P was low as it was crossreactive among rat, hamster, and human.

摘要

一种分子量为26,000且等电点为6.7的多肽,在化学致癌物诱导产生的大鼠肝脏增生性结节(HN)中显著增加,经免疫化学鉴定为从胎盘纯化的中性谷胱甘肽(GSH)转移酶(GSHTase;RX:谷胱甘肽R转移酶,EC 2.5.1.18;也称为GSH S转移酶)的亚基,并经免疫组织化学证明定位于癌前病灶和HN中。在本研究中,已从含HN的肝脏中纯化出GSHTase-P,并使用抗GSHTase-P抗体对其分布和诱导性进行了定量检测。从含HN的肝脏中分离的mRNA进行体外翻译也证实了含HN的肝脏中GSHTase-P的升高。纯化的GSHTase-P大小均一,但在二维凝胶电泳上有两种电荷异构体。在包括肝脏、胎盘和胎儿肝脏在内的正常组织中,GSHTase-P的蛋白质含量通常较低,但在肾脏和胰腺中显著较高。相比之下,含HN的肝脏(原发性肝癌)和可移植的莫里斯肝癌5123D中GSHTase-P的含量比正常肝脏高几十倍,但在可移植的吉田腹水肝癌AH 130中含量低至检测不到。与普通药物代谢酶不同,在癌前病灶和HN出现之前,给予药物和致癌物不会诱导GSHTase-P。此外,GSHTase-P的种属特异性较低,因为它在大鼠、仓鼠和人类之间具有交叉反应性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/59b4/397914/b0a7f087dc1d/pnas00352-0025-a.jpg

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