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PMID 12151437
Gene Name AMH
Condition Sertoli cell-only syndrome, maturation arrest
Association The absence of M2A and AMH immunoreactivity in adult gonads was observed without any correlation to spermatogenetic impairment or molecular deficit in the AZF region. In the samples of these two series, Sertoli cells showed a mature phenotype for AMH and
PMID 12151437
Gene Name AMH
Condition Sertoli cell-only syndrome, maturation arrest
Association The absence of M2A and AMH immunoreactivity in adult gonads was observed without any correlation to spermatogenetic impairment or molecular deficit in the AZF region. In the samples of these two series, Sertoli cells showed a mature phenotype for AMH and
Mutation AZF microdeletions
Population size 39
Population details 39 patients with non-obstructive azoospermia
Sex Male
Infertility type Male infertility
Associated genes AMH, M2A
Other associated phenotypes Sertoli cell-only syndrome, maturation arrest


Absence of anti-Müllerian hormone (AMH) and M2A immunoreactivities in Sertoli cell-only syndrome and maturation arrest with and without AZF microdeletions

Blagosklonova O, Joanne C, Roux C, Bittard H, Fellmann F, Bresson JL.

BACKGROUND: Some genes identified in the AZF locus are expressed only in germinal cells; others are ubiquitous. AZF microdeletions seem to occur at the earliest stages of ontogenetic development, and one might therefore assume that Sertoli cells preserve some immature characteristics and that their immunophenotype may be modified by the existence of a molecular defect. MATERIALS AND METHODS: Two immunohistological markers of Sertoli cell immaturity [anti-Müllerian hormone (AMH) and M2A] were tested in two histopathological groups (maturation arrest at spermatocyte I stage and Sertoli cell-only syndrome). We analysed 68 testicular samples obtained from 39 patients with non-obstructive azoospermia associated or not with AZF microdeletions. RESULTS: The absence of M2A and AMH immunoreactivity in adult gonads was observed without any correlation to spermatogenetic impairment or molecular deficit in the AZF region. In the samples of these two series, Sertoli cells showed a mature phenotype for AMH and M2A markers. CONCLUSIONS: In patients with AZF microdeletions, the genotype-phenotype correlations seem to be more complex than has been suggested previously; more detailed characterization of the immunohistochemical phenotype associated with the molecular defect may be useful in understanding the spermatogenic failure mechanism. FAU - Blagosklonova, O AU - Blagosklonova O AD - Service de Cytogénétique-Immunocytologie-Biologie du Développement et de la Reproduction , CHU et EA MENRT 3185, Faculté de Médecine et de Pharmacie, Place Saint-Jacques, 25030 Besancion Cedex, France. oxana_blagokl@hotmail.com FAU - Joanne, C AU - Joanne C FAU - Roux, C AU - Roux C FAU - Bittard, H AU - Bittard H FAU - Fellmann, F AU - Fellmann F