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POU5F1(OCT-3/4)在正常及发育异常的人类性腺中的发育表达。

Developmental expression of POU5F1 (OCT-3/4) in normal and dysgenetic human gonads.

作者信息

Rajpert-De Meyts Ewa, Hanstein Regina, Jørgensen Niels, Graem Niels, Vogt Peter H, Skakkebaek Niels E

机构信息

Department of Growth & Reproduction, Copenhagen University Hospital (Rigshospitalet), Copenhagen, Denmark.

出版信息

Hum Reprod. 2004 Jun;19(6):1338-44. doi: 10.1093/humrep/deh265. Epub 2004 Apr 22.

Abstract

BACKGROUND

To investigate how long fetal germ cells retain pluripotency, which may be linked to their ability to transform into histologically variable tumours, we examined the expression of OCT-3/4 (POU5F1), a transcription factor essential for the maintenance of totipotency in embryonic stem cells.

METHODS

The ontogeny of expression of OCT-3/4 was studied in 74 specimens of normal human gonads during development and in 58 samples of gonads from cases with testicular dysgenesis syndrome (TDS), including disorders of sex differentiation and malignant changes.

RESULTS

OCT-3/4 expression was found in primordial germ cells during migration to the gonadal ridges and in the indifferent gonad. The expression in testes gradually decreased until approximately 20 weeks of gestation, and thereafter it was more rapidly down-regulated, but persisted in a few cells until 3-4 months of postnatal age, which coincides with the final differentiation of gonocytes into infantile spermatogonia. Subsequently, OCT-3/4 was not detected in normal testes. In the ovaries, OCT-3/4 was expressed in primordial oogonia, but was down-regulated in oocytes that formed primary follicles. The pattern of expression was heterogeneous in dysgenetic and intersex cases, with OCT-3/4-positive gonocytes detected in this series until 14 months of age. Visibly neoplastic gonadoblastoma and carcinoma in situ (CIS) expressed abundant OCT-3/4 regardless of the age.

CONCLUSIONS

In the human ovary, OCT-3/4 is silenced at the onset of the first meiotic prophase, whereas in the testis, down-regulation of OCT-3/4 is a gradual process associated with differentiation of gonocytes. This normal pattern of expression is disturbed in dysgenetic gonads, especially in rare intersex cases, thus increasing the risk of malignant transformation. The high abundance of OCT-3/4 in CIS cells is consistent with their early fetal origin and pluripotency.

摘要

背景

为了研究胎儿生殖细胞保持多能性的时间长度,这可能与其转化为组织学上可变肿瘤的能力相关,我们检测了OCT-3/4(POU5F1)的表达,OCT-3/4是维持胚胎干细胞全能性所必需的转录因子。

方法

研究了74例发育过程中正常人类性腺标本以及58例睾丸发育不全综合征(TDS)患者性腺标本中OCT-3/4的表达情况,TDS包括性分化障碍和恶性病变。

结果

在原始生殖细胞迁移至性腺嵴以及未分化性腺中发现有OCT-3/4表达。睾丸中的表达逐渐降低,直至妊娠约20周,此后其下调速度加快,但在少数细胞中持续存在至出生后3 - 4个月,这与生殖母细胞最终分化为婴儿型精原细胞的时间一致。随后,在正常睾丸中未检测到OCT-3/4。在卵巢中,OCT-3/4在原始卵原细胞中表达,但在形成初级卵泡的卵母细胞中下调。在发育异常和两性畸形病例中,表达模式是异质性的,在该系列病例中直到14个月龄仍可检测到OCT-3/4阳性生殖母细胞。明显的肿瘤性腺母细胞瘤和原位癌(CIS)无论年龄大小均表达丰富的OCT-3/4。

结论

在人类卵巢中,OCT-3/4在第一次减数分裂前期开始时沉默,而在睾丸中,OCT-3/4的下调是一个与生殖母细胞分化相关的渐进过程。这种正常的表达模式在发育异常的性腺中受到干扰,尤其是在罕见的两性畸形病例中,从而增加了恶性转化的风险。CIS细胞中OCT-3/4的高丰度与其早期胎儿起源和多能性一致。

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