Document details

Incorrect DNA methylation of the DAZL promoter CpG island associates with defec...

Author(s): Navarro-Costa, Paulo cv logo 1 ; Nogueira, Paulo cv logo 2 ; Carvalho, Marta cv logo 3 ; Leal, Fernanda cv logo 4 ; Cordeiro, Inês cv logo 5 ; Calhaz-Jorge, Carlos cv logo 6 ; Gonçalves, João cv logo 7 ; Plancha, Carlos E. cv logo 8

Date: 2010

Persistent ID: http://hdl.handle.net/10400.18/118

Origin: Repositório Científico do Instituto Nacional de Saúde

Subject(s): Male infertility; Spermatogenesis; Epigenetics; DAZ gene family; DNA methylation; Doenças Genéticas; Determinantes da Saúde e da Doença; Estados de Saúde e de Doença


Description
Versão impressa: Hum Reprod. 2010 Oct;25(10):2647-54 Background: Successful gametogenesis requires the establishment of an appropriate epigenetic state in developing germ cells. Nevertheless, an association between abnormal spermatogenesis and epigenetic disturbances in germline-specific genes remains to be demonstrated. Methods: In this study, the DNA methylation pattern of the promoter CpG island (CGI) of two germline regulator genes—DAZL and DAZ, was characterized by bisulphite genomic sequencing in quality-fractioned ejaculated sperm populations from normozoospermic (NZ) and oligoasthenoteratozoospermic (OAT) men. Results: OAT patients display increased methylation defects in the DAZL promoter CGI when compared with NZ controls. Such differences are recorded when analyzing sperm fractions enriched either in normal or defective germ cells (P , 0.001 in both cases). Significant differences in DNA methylation profiles are also observable when comparing the qualitatively distinct germ cell fractions inside the NZ and OAT groups (P ¼ 0.003 and P ¼ 0.007, respectively). Contrastingly, the unmethylation pattern of the DAZ promoter CGI remains correctly established in all experimental groups. Conclusions: An association between disrupted DNA methylation of a key spermatogenesis gene and abnormal human sperm is described here for the first time. These results suggest that incorrect epigenetic marks in germline genes may be correlated with male gametogenic defects.
Document Type Article
Language English
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