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卵丘细胞是老年小鼠卵母细胞凋亡潜能增加所必需的。

Cumulus cells are required for the increased apoptotic potential in oocytes of aged mice.

作者信息

Perez G I, Tilly J L

机构信息

Vincent Center for Reproductive Biology, Department of Obstetrics and Gynecology, Massachusetts General Hospital/Harvard Medical School, Boston 02114, USA.

出版信息

Hum Reprod. 1997 Dec;12(12):2781-3. doi: 10.1093/humrep/12.12.2781.

Abstract

Recent studies with female ICR mice have suggested that oocyte DNA fragmentation is one reason for poor oocyte quality and lower fertility associated with ageing. Since it was not determined if this increased 'apoptotic' potential in aged oocytes is due to changes within the oocyte itself or within the microenvironment of cumulus cells (CC) surrounding the germ cell, we sought to clarify if CC were required to affect the rate of apoptosis in oocytes maintained in vitro. Intact cumulus-oocyte complexes (COC) were retrieved by superovulation of virgin female ICR mice at 7 weeks ('young') or 34-35 weeks ('aged') of age. One-half of the COC in each group were incubated at 37 degrees C in human tubal fluid medium under paraffin oil for 24 h. The other half of the COC in each group were denuded of CC and incubated under the same conditions (denuded oocytes; DO). Following incubation, COC were stripped of adherent CC by gentle pipetting. All DO were then fixed and checked by light microscopy for morphological changes characteristic of apoptosis. In young mice, the presence of CC had no significant effect on oocyte death rate (18 +/- 9% and 14 +/- 6% apoptotic oocytes in COC and DO, respectively; P > 0.05). However, in aged mice the percentage of CC-enclosed oocytes that underwent apoptosis was significantly greater as compared to the death rate in DO (48 +/- 3% versus 19 +/- 8% apoptotic oocytes, respectively; P < 0.05). This increased death potential was due to the presence of CC since the occurrence of apoptosis in DO of aged versus young mice was not significantly different (19 +/- 8% versus 14 +/- 6% apoptotic oocytes, respectively; P > 0.05). These results demonstrate that the age-dependent acceleration of apoptosis in oocytes maintained in vitro requires the CC.

摘要

最近对雌性ICR小鼠的研究表明,卵母细胞DNA片段化是卵母细胞质量差以及与衰老相关的生育力降低的一个原因。由于尚未确定衰老卵母细胞中这种增加的“凋亡”潜能是由于卵母细胞自身的变化还是由于围绕生殖细胞的卵丘细胞(CC)微环境中的变化,我们试图阐明CC是否是影响体外培养的卵母细胞凋亡率所必需的。通过对7周龄(“年轻”)或34 - 35周龄(“衰老”)的未交配雌性ICR小鼠进行超排卵来获取完整的卵丘 - 卵母细胞复合体(COC)。每组中一半的COC在37℃下于石蜡油覆盖的人输卵管液培养基中孵育24小时。每组中另一半的COC去除CC后在相同条件下孵育(裸卵;DO)。孵育后,通过轻柔吹打去除COC上附着的CC。然后将所有DO固定并通过光学显微镜检查凋亡的形态学特征。在年轻小鼠中,CC的存在对卵母细胞死亡率没有显著影响(COC和DO中凋亡卵母细胞分别为18±9%和14±6%;P>0.05)。然而,在衰老小鼠中,与DO中的死亡率相比,被CC包裹的卵母细胞发生凋亡的百分比显著更高(分别为48±3%和19±8%凋亡卵母细胞;P<0.05)。这种增加的死亡潜能是由于CC的存在,因为衰老与年轻小鼠的DO中凋亡的发生率没有显著差异(分别为19±8%和14±6%凋亡卵母细胞;P>0.05)。这些结果表明,体外培养的卵母细胞中与年龄相关的凋亡加速需要CC。

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