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通过精原干细胞移植恢复辐射青春期恒河猴的功能性精子生成。

Restoration of functional sperm production in irradiated pubertal rhesus monkeys by spermatogonial stem cell transplantation.

机构信息

Department of Experimental Radiation Oncology, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA.

Department of Veterinary Medicine and Surgery, The University of Texas MD Anderson Cancer Center, Houston, Texas, USA.

出版信息

Andrology. 2020 Sep;8(5):1428-1441. doi: 10.1111/andr.12807. Epub 2020 May 18.

Abstract

BACKGROUND

In male pre-pubertal cancer patients, radiation and chemotherapy impact future fertility by eradication of spermatogonial stem cells (SSCs). In macaques, spermatogenesis could be regenerated by intratesticular transplantation of SSCs, but only a small percentage of spermatozoa produced were of donor origin. Transient hormone suppression with a GnRH antagonist (GnRH-ant) enhanced spermatogenic recovery from transplanted SSCs.

OBJECTIVES

To evaluate donor-derived and endogenous spermatogenic recovery after SSC transplantation into irradiated monkeys and to test whether hormone suppression around the time of transplantation facilitates spermatogenic recovery.

MATERIALS AND METHODS

Testes of 15 adult rhesus monkeys were irradiated with 7 Gy and 4 months later transplanted, to one of the testes, with cryopreserved testicular cells containing SSCs from unrelated monkeys. Monkeys were either treated with GnRH-ant for 8 weeks before transplantation, GnRH-ant from 4 weeks before to 4 weeks after transplantation, or with no GnRH-ant. Tissues were harvested 10 months after transplantation.

RESULTS

Two of the 15 monkeys, a control and a pre-transplantation GnRH-ant-treated, showed substantially higher levels of testicular spermatogenesis and epididymal sperm output in the transplanted side as compared to the untransplanted. Over 84% of epididymal spermatozoa on the transplanted side had the donor genotype and were capable of fertilizing eggs after intracytoplasmic sperm injection forming morulae of the donor paternal origin. Low levels of donor spermatozoa (~1%) were also identified in the epididymis of three additional monkeys. Transplantation also appeared to enhance endogenous spermatogenesis.

DISCUSSION AND CONCLUSION

We confirmed that SSC transplantation can be used for restoration of fertility in male cancer survivors exposed to irradiation as a therapeutic agent. The success rate of this procedure, however, is low. The success of filling the tubules with the cell suspension, but not the GnRH-ant treatment, was related to the level of colonization by transplanted cells.

摘要

背景

在男性青春期前癌症患者中,放射治疗和化学疗法通过消灭精原干细胞(SSC)来影响未来的生育能力。在猕猴中,通过将 SSC 进行睾丸内移植,可以使精子发生再生,但产生的精子只有一小部分来自供体。用 GnRH 拮抗剂(GnRH-ant)进行短暂的激素抑制可增强移植 SSC 的生精恢复。

目的

评估 SSC 移植到受照射猕猴后供体源性和内源性精子发生的恢复情况,并测试移植前后激素抑制是否有利于精子发生的恢复。

材料和方法

15 只成年恒河猴的睾丸接受 7Gy 照射,4 个月后,将来自无关猕猴的冷冻睾丸细胞(包含 SSC)移植到一侧睾丸。猴子在移植前 8 周接受 GnRH-ant 治疗,或在移植前 4 周至移植后 4 周接受 GnRH-ant 治疗,或不接受 GnRH-ant 治疗。在移植后 10 个月采集组织。

结果

在 15 只猴子中,有 2 只(一只对照,一只移植前 GnRH-ant 处理)的移植侧睾丸精子发生和附睾精子输出明显高于未移植侧。超过 84%的移植侧附睾精子具有供体基因型,并且能够在胞浆内精子注射后使卵子受精,形成供体父系来源的桑葚胚。在另外 3 只猴子的附睾中也鉴定出低水平的供体精子(~1%)。移植似乎也增强了内源性精子发生。

讨论与结论

我们证实 SSC 移植可用作治疗男性癌症幸存者暴露于辐射后的生育力恢复的治疗剂。然而,该程序的成功率较低。细胞悬液填充管腔的成功率,而不是 GnRH-ant 治疗的成功率,与移植细胞的定植水平有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a0ac/7521830/76dd48e5bc6d/nihms-1621925-f0001.jpg

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