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卵巢卵泡巨噬细胞:未成熟大鼠的卵泡闭锁是巨噬细胞介导的事件吗?

Ovarian follicle macrophages: is follicular atresia in the immature rat a macrophage-mediated event?

作者信息

Gaytán F, Morales C, Bellido C, Aguilar E, Sánchez-Criado J E

机构信息

Department of Cell Biology, Faculty of Medicine, University of Córdoba, Spain.

出版信息

Biol Reprod. 1998 Jan;58(1):52-9. doi: 10.1095/biolreprod58.1.52.

Abstract

Macrophages have recently been found to play roles in most ovarian events through cytokine release and/or cell-cell communication. We studied the presence of macrophages in the ovaries of neonatal (0-7 days of age), juvenile (10-20 days of age), and prepubertal (25-30 days of age) rats, as well as adult cycling rats, in relation to follicular development and atresia. Macrophages were extremely scarce in the ovarian stroma up to 30 days of age. However, at 10 days of age, about 13% of small growing healthy follicles contained macrophages among granulosa cells. The percentage of macrophage-containing follicles at 15 days of age was about 60%, and the vast majority of these follicles also had pyknotic granulosa cells, which increased in number from 15 to 20 days of age. This type of atresia showed distinctive morphological and functional features in comparison with the atretic process observed in adult cycling rats. At 25 and 30 days of age, atretic follicles in advanced stages of atresia, together with atretic follicles similar to those present in adult rats, were observed. In adult rats, only a small proportion of healthy growing follicles contained macrophages. These cells were absent from early atretic follicles, and invasion by macrophages occurred at advanced stages of atresia. These data indicate that a different type of atresia occurred during early postnatal development, probably related to the special endocrine environment in immature rats. The close association between the presence of macrophages inside the follicles and of apoptotic granulosa cells strongly supports the hypothesis that macrophages mediate follicular atresia in immature rats.

摘要

最近发现巨噬细胞通过细胞因子释放和/或细胞间通讯在大多数卵巢事件中发挥作用。我们研究了新生(0至7日龄)、幼年(10至20日龄)、青春期前(25至30日龄)大鼠以及成年周期性发情大鼠卵巢中巨噬细胞的存在情况,及其与卵泡发育和闭锁的关系。直至30日龄,卵巢基质中的巨噬细胞极其稀少。然而,在10日龄时,约13%正在生长的健康小卵泡的颗粒细胞中含有巨噬细胞。15日龄时含巨噬细胞的卵泡百分比约为60%,并且这些卵泡中的绝大多数也有固缩的颗粒细胞,其数量在15至20日龄时增加。与成年周期性发情大鼠中观察到的闭锁过程相比,这种闭锁类型表现出独特的形态和功能特征。在25和30日龄时,观察到处于闭锁晚期的闭锁卵泡,以及与成年大鼠中存在的类似的闭锁卵泡。在成年大鼠中,只有一小部分健康生长的卵泡含有巨噬细胞。早期闭锁卵泡中没有这些细胞,巨噬细胞在闭锁晚期侵入。这些数据表明,在出生后早期发育过程中发生了一种不同类型的闭锁,可能与未成熟大鼠的特殊内分泌环境有关。卵泡内巨噬细胞的存在与凋亡颗粒细胞的密切关联有力地支持了巨噬细胞介导未成熟大鼠卵泡闭锁的假说。

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