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Mtor inhibition by INK128 extends functions of the ovary reconstituted from germline stem cells in aging and premature aging mice

机译:MTOR通过INK128抑制卵巢从老化和过早老化小鼠中从种系干细胞重构的卵巢的功能

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摘要

Stem cell transplantation has been generally considered as promising therapeutics in preserving or recovering functions of lost, damaged, or aging tissues. Transplantation of primordial germ cells (PGCs) or oogonia stem cells (OSCs) can reconstitute ovarian functions that yet sustain for only short period of time, limiting potential application of stem cells in preservation of fertility and endocrine function. Here, we show that mTOR inhibition by INK128 extends the follicular and endocrine functions of the reconstituted ovaries in aging and premature aging mice following transplantation of PGCs/OSCs. Follicular development and endocrine functions of the reconstituted ovaries by transplanting PGCs into kidney capsule of the recipient mice were maintained by INK128 treatment for more than 12 weeks, in contrast to the controls for only about 4 weeks without receiving the mTOR inhibitors. Comparatively, rapamycin also can prolong the ovarian functions but for limited time. Furthermore, our data reveal that INK128 promotes mitochondrial function in addition to its known function in suppression of immune response and inflammation. Taken together, germline stem cell transplantation in combination with mTOR inhibition by INK128 improves and extends the reconstituted ovarian and endocrine functions in reproductive aging and premature aging mice.
机译:干细胞移植通常被认为是有前途的治疗方法,用于保存或恢复丢失,损坏或老化组织的功能。原始胚芽细胞(PGCs)或oogonia干细胞(OSCs)的移植可以重组卵巢官能团,其仅仅是短时间,限制干细胞在保存生育和内分泌功能中的潜在应用。在此,我们表明MTOR通过INK128抑制在移植PGCS / OSC后的衰老和过早老化小鼠中延伸了重构卵巢的滤窗和内分泌功能。通过将PGC移植到受体小鼠的肾脏胶囊中,通过Ink 128治疗将重构卵形的卵泡发育和内分泌功能通过Ink128治疗超过12周,与对照组仅约4周,而不接受MTOR抑制剂。相比之下,雷帕霉素也可以延长卵巢功能,但时间有限。此外,我们的数据表明,除了抑制免疫应答和炎症时,还促进Ink128促进线粒体功能。一起服用,种系干细胞移植与油墨128的MTOR抑制相结合,可改善并延伸生殖衰老和过早老化小鼠中的重构卵巢和内分泌功能。

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