Development of KISS1 knockout pigs is characterized by hypogonadotropic hypogonadism, normal growth, and reduced skatole†.

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Daniel F Ahern, Kyra Martins, Julio M Flórez, Caitlin E Ross, Abe Huisman, Robert A Cushman, Sydney L Shuping, Casey C Nestor, Amy T Desaulniers, Brett R White, Tad S Sonstegard, Clay A Lents
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Abstract

Kisspeptin is a major regulator of gonadotropin secretion in pigs. Previously, CRISPR/Cas9 knockout of KISS1 was used to develop a mosaic parental line of pigs to generate offspring that would not need castration due to loss of kisspeptin. The current goal was to characterize growth and reproductive development of F1 pigs from this parental line. Body weights, gonadotropin concentrations and gonadal development were measured from birth through development (boars to 220 days of age, n = 42; gilts to 160 days of age, n = 36). Testosterone, skatole, and androstenone were also measured in boars. Blood samples were collected by jugular venipuncture for quantification of serum hormones, gonadal tissues were collected for gross morphology and histology, and a fat biopsy was collected (boars) for skatole and androstenone analysis. Body weight did not differ with genotype. There were no differences between KISS1+/+ and heterozygote KISS1+/- animals for most parameters measured. Gonadotropin concentrations were reduced in KISS1-/- boars and gilts compared with KISS1+/+ and KISS1+/- animals (P < 0.05). Concentrations of testosterone in serum and both androstenone and skatole in adipose were less in KISS1-/- boars than in KISS1+/+ and KISS1+/- boars (P < 0.05). Hypogonadism was present in all KISS1-/- gilts and boars. These data indicate that knocking out KISS1 causes hypogonadotropic hypogonadism but does not negatively affect growth in pigs. Only one KISS1 allele is needed for normal gonadotropin secretion and gonadal development, and accumulation of compounds in adipose leading to boar taint.

KISS1 基因敲除猪的发育特点是性腺功能减退、生长正常和皮脂减少。
Kisspeptin 是猪促性腺激素分泌的主要调节因子。在此之前,我们曾利用 CRISPR/Cas9 敲除 KISS1 的方法培育了一个马赛克亲本猪品系,以产生不需要因丧失 Kisspeptin 而进行阉割的后代。目前的目标是鉴定来自该亲本品系的 F1 猪的生长和生殖发育特征。我们测量了从出生到发育期间的体重、促性腺激素浓度和性腺发育情况(公猪至 220 日龄,n = 42;后备母猪至 160 日龄,n = 36)。此外,还测定了公猪的睾酮、睾酮和雄烯酮。通过颈静脉穿刺采集血液样本用于血清激素的定量分析,采集性腺组织用于大体形态学和组织学研究,并采集脂肪活检样本(公猪)用于睾酮和雄酮的分析。体重与基因型没有差异。KISS1+/+和杂合子KISS1+/-动物的大多数测量参数没有差异。与 KISS1+/+ 和 KISS1+/- 动物相比,KISS1-/- 公猪和后备母猪的促性腺激素浓度降低(P
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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