Testosterone production begins at weeks 8 to 9 of gestation in the human; this a critical event for primary male sexual development in a 46,XY embryo (masculinization), and for normal secondary sexual development at puberty (virilization). Testosterone also is essential to maintain the secondary sexual characters during adulthood, and for the initiation and preservation of spermatogenesis. The androgen actions are mediated by the androgen receptor (AR). Upon binding of androgens to its receptor, the AR undergoes a conformational change that converts it from an inactive state to its active DNA-binding state. In the human testis, the AR immunoexpression has been detected exclusively in the Sertoli cells nuclei, in the Leydig cells, and in the peritubular myoid cells. These cells function have an strong relation with the AR concentration and expression. Mutations of the AR results in alteration of androgens actions, affecting the endocrine function at the testicular level and in other target organs, affecting also the reproductive function. The meaningful of the AR expression in the congenital and acquired functional testicular pathology, has not been established yet. In this review different immunohistochemical expression patterns of the AR, reported in the testis from normal men, and from patients with testicular pathology are evaluated; also the functional significance from the histological and molecular alterations of the AR are evaluated, in relation with the fertility dysfunction of these patients.