Mouse oocytes injected with testicular spermatozoa or round spermatids can develop into normal offspring

生物 精子细胞 男科 原核 后代 精子发生 印记(心理学) 基因组印记 胚胎 配子发生 精子 人类受精 生殖技术 精子发生 胚胎干细胞 施肥 生殖细胞 胚胎发生 遗传学 内分泌学 合子 基因 基因表达 怀孕 DNA甲基化 医学
作者
Yasuyuki Kimura,Ryuzo Yanagimachi
出处
期刊:Development [The Company of Biologists]
卷期号:121 (8): 2397-2405 被引量:396
标识
DOI:10.1242/dev.121.8.2397
摘要

Genomic imprinting occurs in both male and female gametes during gametogenesis, but the exact time when imprinting begins and ends is unknown. In the present study we injected nuclei of testicular spermatozoa and round spermatids into mature mouse oocytes to see whether these nuclei are able to participate in syngamy and normal embryonic development. If the injected oocytes develop into normal fertile offspring, imprinting in the male germ cells used must have been completed by the time of injection. Ninety-two percent of mouse oocytes injected with testicular spermatozoa survived and 94% of these were fertilized normally (extrusion of the second polar body and formation of male and female pronuclei). When 44 two-cell embryos so created were transferred to 5 foster mothers, 24 (54.5%) developed into normal offspring. Unlike testicular spermatozoa, round spermatids could not activate the oocytes, and therefore the oocytes had to be activated artificially either before or after spermatid injection. The highest rate (77%) of normal fertilization was obtained when the oocytes were first activated by electric current, then injected individually with a single spermatid nucleus. When 131 two-cell embryos were transferred to 15 foster mothers, 37 (28.2%) reached full term. All but two grew into healthy adults. Thus, it would appear that gametic imprinting in mouse spermatogenic cells is completed before spermiogenesis begins. Under the experimental conditions employed, spermatid nuclei were less efficient than testicular sperm nuclei in producing normal offspring, but perhaps this was due to technical rather than inherent problems.
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