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The Autoimmune Regulator (AIRE) preserves fertility in male and female Balb/c mice.

机译:自身免疫调节剂(AIRE)保持雄性和雌性Balb / c小鼠的生育力。

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摘要

The Autoimmune Regulator (AIRE) contributes to central immune tolerance through the induction of self-antigen expression within the thymus. In humans, a defect in AIRE results in a multi-organ autoimmune disorder known as Autoimmune Polyglandular Syndrome Type-1. Both humans and mice with a deficiency in this gene develop autoreactive CD4+ T cells, serum autoantibodies and elevated rates of infertility. Interestingly, the pathology of autoimmune infertility in Aire-deficient (Aire-KO) mice differs between males and females. Ovarian autoimmunity causing a depletion of follicular reserves is prominent in female Aire-KO mice over 10 weeks of age. However, 50% of mated six-week old female Aire -KO mice demonstrate embryo loss by embryonic day (ED) 7.5 despite having normal follicular reserves. We determined that ovulation (90% KO vs 100% WT; n=11), mating frequency (99% KO vs 100% WT; n>58), progesterone production (p=0.232; n=4) and decidualization are unaffected. However, 60% (9 of 15) of 6-8 week old Aire-KO female mice generated serum autoantibodies against the ovary and more frequently ovulated degenerated oocytes (31% KO vs 2% WT; n>71) When cultured, one-cell embryos from Aire-KO females failed to become 2-cell and blastocyst stage embryos at significantly reduced rate compared to WT controls (47% KO vs 76% WT and 19% KO vs 60% WT; n>67). Finally, embryos from Aire-KO dams are developmentally delayed at ED3.5 with a reduced trophectoderm outgrowth potential after 48 and 96 hours of culture (0mm2 KO vs 7.1 mm2 WT, and 16.5 mm2 KO vs 30.9 mm2 WT; p<0.001, n=4). Alternatively, male Aire-KO mice have greater variability in the autoimmune targets associated with reduced fertility (18% KO vs 80% WT; n=10). Signs of disease included reduced testosterone (p=0.03; n=18), loss of vomeronasal organ-associated glands (86% KO vs 0% WT; n=7), prostatitis (90% KO vs 0% WT; n=20), epididymitis (75% KO vs 0% WT; n=20) and reduced in vitro fertilization rates (9% KO vs 54% WT; n>83 oocytes). Additionally a subset of males (23%; n=22) exhibited oligozoospermia with disruption of the blood-testis barrier. Collectively these results demonstrate the importance of central immune tolerance on fertility preservation by preventing autoimmune disease against the male and female reproductive systems.
机译:自身免疫调节剂(AIRE)通过诱导胸腺内自身抗原的表达来促进中枢免疫耐受。在人类中,AIRE缺陷会导致多器官自身免疫性疾病,称为自身免疫性多腺综合征1型。缺乏该基因的人类和小鼠都会发展自身反应性CD4 + T细胞,血清自身抗体和不孕率升高。有趣的是,雄性和雌性在缺乏Aire的(Aire-KO)小鼠中自身免疫性不育的病理学有所不同。导致卵泡储备耗尽的卵巢自身免疫在10周龄以上的雌性Aire-KO小鼠中尤为突出。但是,尽管卵泡储备正常,但有50%的六周龄雌性Aire -KO小鼠表现出胚胎天数(ED)7.5丧失胚胎。我们确定排卵(90%KO对100%WT; n = 11),交配频率(99%KO对100%WT; n> 58),孕酮生成(p = 0.232; n = 4)和蜕膜不受影响。但是,在6-8周大的Aire-KO雌性小鼠中,有60%(15个中的9个)产生了针对卵巢的血清自身抗体,并且排卵的变性卵母细胞频率更高(31%KO对2%WT; n> 71)。与野生型对照相比,来自Aire-KO雌性的细胞胚胎未能以显着降低的速率变成2细胞和胚泡期胚胎(47%KO vs 76%WT和19%KO vs 60%WT; n> 67)。最后,在培养48和96小时后,Aire-KO大坝的胚胎在ED3.5发育延迟,滋养外胚层的生长潜力降低(0mm2 KO vs 7.1 mm2 WT,16.5 mm2 KO vs 30.9 mm2 WT; p <0.001,n = 4)。或者,雄性Aire-KO小鼠的自身免疫性靶标中与生育力降低相关的变异性更大(18%KO对80%WT; n = 10)。疾病迹象包括睾丸激素降低(p = 0.03; n = 18),与犁鼻器官相关的腺体丢失(86%KO vs 0%WT; n = 7),前列腺炎(90%KO vs 0%WT; n = 20) ),附睾炎(75%KO vs 0%WT; n = 20)和体外受精率降低(9%KO vs 54%WT; n> 83卵母细胞)。另外,有一部分男性(23%; n = 22)表现出少精子症,并破坏了血液-睾丸屏障。这些结果共同证明了通过预防针对男性和女性生殖系统的自身免疫性疾病,中枢免疫耐受对保持生育能力的重要性。

著录项

  • 作者

    Warren, Bryce D.;

  • 作者单位

    University of Kansas.;

  • 授予单位 University of Kansas.;
  • 学科 Immunology.;Cellular biology.
  • 学位 Ph.D.
  • 年度 2014
  • 页码 195 p.
  • 总页数 195
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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