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Summary. The responsiveness of decapsulated testes and isolated Leydig cell preparations from rats (30–80 days of age) to a constant dose of 3 ng hCG/2 ml was assessed by comparison of the production of testosterone and 'total 17β-hydroxy androgen' (17β-HA). When testosterone secretion was used as the index of response, there was a marked increase in the production with age by decapsulated testes and also by equal numbers of Leydig cells. When 17β-HA was taken as the response parameter this increase was only marginal for the decapsulated testes and there was an age-dependent decrease when expressed per 106 cells. These differences probably reflect changes in the metabolism of testosterone to 5
-reduced products with increasing age because 80% of androgen secreted at 30 days is 3-androstanediol and 86% is secreted as testosterone at 80 days. We conclude that for studies on hCG responsiveness and the steroidogenic capacity of immature rat Leydig cells (a) testosterone is an inappropriate response parameter and (b) this response undergoes a decrease rather than an increase during prepubertal development.
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