Department of Genetics and Animal Breeding, Poznan University of Life Sciences, Poznan, Poland.
Sex Dev. 2012;6(1-3):128-34. doi: 10.1159/000330921. Epub 2011 Aug 30.
Hypospadias is rarely reported in dogs. In this study we pre-sent 2 novel cases of this disorder of sexual development and, in addition, a case of hereditary sex reversal in a female with an enlarged clitoris. The first case was a male Moscow watchdog with a normal karyotype (78,XY) and the presence of the SRY gene. In this dog, perineal hypospadias, bilateral inguinal cryptorchidism and testes were observed. The second case, representing the Cocker spaniel breed, had a small penis with a hypospadic orifice of the urethra, bilateral cryptorchidism, testis and a rudimentary gonad inside an ovarian bursa, a normal female karyotype (78,XX) and a lack of the SRY gene. This animal was classified as a compound sex reversal (78,XX, SRY-negative) with the hypospadias syndrome. The third case was a Cocker spaniel female with an enlarged clitoris and internally located ovotestes. Cytogenetic and molecular analyses revealed a normal female karyotype (78,XX) and a lack of the SRY gene, while histology of the gonads showed an ovotesticular structure. This case was classified as a typical hereditary sex reversal syndrome (78,XX, SRY-negative). Molecular studies were focused on coding sequences of the SRY gene (case 1) and 2 candidates for monogenic hypospadias, namely MAMLD1 (mastermind-like domain containing 1) and SRD5A2 (steroid-5-alpha-reductase, alpha polypeptide 2). Sequencing of the entire SRY gene, including 5'- and 3'-flanking regions, did not reveal any mutation. The entire coding sequence of MAMLD1 and SRD5A2 was analyzed in all the intersexes, as well as in 4 phenotypically normal control dogs (3 females and 1 male). In MAMLD1 2 SNPs, including 1 missense substitution in exon 1 (c.128A>G, Asp43Ser), were identified, whereas in SRD5A2 7 polymorphisms, including 1 missense SNP (c.358G>A, Ala120Thr), were found. None of the identified polymorphisms cosegregated with the intersexual phenotype, thus, we cannot confirm that hypospadias may be associated with polymorphism in the coding sequence of the studied genes.
尿道下裂在犬中很少见。在本研究中,我们介绍了 2 例这种性发育障碍的新病例,以及一例具有增大阴蒂的遗传性性别反转的雌性病例。第一例是一只莫斯科看门犬,具有正常的核型(78,XY)和 SRY 基因的存在。在这只狗中,观察到会阴尿道下裂、双侧腹股沟隐睾和睾丸。第二例是可卡犬品种,具有小阴茎,尿道下裂口,双侧隐睾,睾丸和卵巢囊中一个发育不全的生殖腺,正常的女性核型(78,XX)和缺乏 SRY 基因。该动物被归类为复合性别反转(78,XX,SRY-阴性)与尿道下裂综合征。第三例是一只具有增大阴蒂和内部卵睾的可卡犬雌性。细胞遗传学和分子分析显示正常的女性核型(78,XX)和缺乏 SRY 基因,而性腺组织学显示卵睾结构。该病例被归类为典型的遗传性性别反转综合征(78,XX,SRY-阴性)。分子研究集中在 SRY 基因的编码序列(病例 1)和 2 个单基因尿道下裂候选基因,即 MAMLD1(类脑发育相关蛋白 1)和 SRD5A2(类固醇-5-α-还原酶,α 多肽 2)。整个 SRY 基因,包括 5'和 3'侧翼区的测序未发现任何突变。所有间性个体以及 4 只表型正常的对照犬(3 只雌性和 1 只雄性)均分析了 MAMLD1 和 SRD5A2 的整个编码序列。在 MAMLD1 中鉴定了 2 个 SNP,包括外显子 1 中的 1 个错义取代(c.128A>G,Asp43Ser),而在 SRD5A2 中鉴定了 7 个多态性,包括 1 个错义 SNP(c.358G>A,Ala120Thr)。鉴定的多态性均未与间性表型共分离,因此,我们不能确认尿道下裂可能与研究基因的编码序列中的多态性有关。
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