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卵泡抑素同工型的差异分布:一种新型FS315特异性免疫测定法的应用

Differential distribution of follistatin isoforms: application of a new FS315-specific immunoassay.

作者信息

Schneyer Alan L, Wang Qifa, Sidis Yisrael, Sluss Patrick M

机构信息

Reproductive Endocrine Unit, Massachusetts General Hospital, Boston, Massachusetts 02114, USA.

出版信息

J Clin Endocrinol Metab. 2004 Oct;89(10):5067-75. doi: 10.1210/jc.2004-0162.

Abstract

Follistatin (FST) is a monomeric activin-binding and neutralization protein that has at least three isoforms in human tissues and fluids. The full-length FS315 protein has an acidic 26-residue C-terminal tail that is not present in the shortest form, FS288, due to alternative splicing. An intermediate form, FS303, was identified in follicular fluid that is presumably derived by proteolytic processing of this tail domain. Interestingly, the biochemistry of each of these three isoforms is distinct, including their ability to bind to cell surface proteoglycans, an activity that ranks in the order FS288 > FS303 > FS315. This would suggest that the soluble, circulating FST isoform is likely to be FS315, a hypothesis supported by previous determinations that the serum and follicular fluid forms of FST are biochemically distinct. To test this hypothesis, we developed an immunoassay that is specific for full-length FS315. This assay was validated for use with human serum and follicular fluid samples and then used to examine FST in these fluid compartments. Our results indicate that FS315 is indeed the major circulating FST isoform but is undetectable in follicular fluid samples aspirated from normal women or women with polycystic ovary syndrome. These observations confirm the compartmentalization of FST isoforms according to their biochemical properties and biological actions so that the most soluble form is found in the circulation, whereas the forms that bind to cell surface proteoglycans are found in tissue compartments such as the ovarian follicle. They also confirm that the source of FST in human serum is not the ovarian follicle.

摘要

卵泡抑素(FST)是一种单体激活素结合和中和蛋白,在人体组织和体液中至少有三种异构体。全长FS315蛋白有一个酸性的26个残基的C末端尾巴,由于选择性剪接,最短形式的FS288中不存在该尾巴。在卵泡液中鉴定出一种中间形式FS303,推测它是由该尾巴结构域的蛋白水解加工产生的。有趣的是,这三种异构体中的每一种的生物化学性质都不同,包括它们与细胞表面蛋白聚糖结合的能力,这种活性的顺序为FS288 > FS303 > FS315。这表明可溶性循环FST异构体可能是FS315,先前的测定支持了这一假设,即FST的血清和卵泡液形式在生物化学上是不同的。为了验证这一假设,我们开发了一种对全长FS315具有特异性的免疫测定法。该测定法经过验证可用于人血清和卵泡液样本,然后用于检测这些液体成分中的FST。我们的结果表明,FS315确实是主要的循环FST异构体,但在从正常女性或多囊卵巢综合征女性中抽取的卵泡液样本中无法检测到。这些观察结果证实了FST异构体根据其生物化学性质和生物学作用进行了区室化,因此在循环中发现了最易溶的形式,而与细胞表面蛋白聚糖结合的形式则存在于组织区室如卵巢卵泡中。它们还证实了人血清中FST的来源不是卵巢卵泡。

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