Painful ovulation in a 46,XX SRY −ve adult male with SOX9 duplication

Author:

Shankara Narayana Nandini12,Kean Anne-Maree1,Ewans Lisa13,Ohnesorg Thomas4,Ayers Katie L45,Watson Geoff1,Vasilaras Arthur1,Sinclair Andrew H45,Twigg Stephen M1,Handelsman David J2

Affiliation:

1. 1Royal Prince Alfred Hospital, Sydney, New South Wales Australia

2. 2ANZAC Research Institute, University of Sydney, Sydney, New South Wales Australia

3. 3Central Clinical School, Sydney Medical School, University of Sydney, New South Wales Australia

4. 4Murdoch Childrens Research Institute, Melbourne, Victoria Australia

5. 5Department of Paediatrics, University of Melbourne, Melbourne, Victoria Australia

Abstract

Summary 46,XX disorders of sexual development (DSDs) occur rarely and result from disruptions of the genetic pathways underlying gonadal development and differentiation. We present a case of a young phenotypic male with 46,XX SRY-negative ovotesticular DSD resulting from a duplication upstream of SOX9 presenting with a painful testicular mass resulting from ovulation into an ovotestis. We present a literature review of ovulation in phenotypic men and discuss the role of SRY and SOX9 in testicular development, including the role of SOX9 upstream enhancer region duplication in female-to-male sex reversal. Learning points: In mammals, the early gonad is bipotent and can differentiate into either a testis or an ovary. SRY is the master switch in testis determination, responsible for differentiation of the bipotent gonad into testis. SRY activates SOX9 gene, SOX9 as a transcription factor is the second major gene involved in male sex determination. SOX9 drives the proliferation of Sertoli cells and activates AMH/MIS repressing the ovary. SOX9 is sufficient to induce testis formation and can substitute for SRY function. Assessing karyotype and then determination of the presence or absence of Mullerian structures are necessary serial investigations in any case of DSD, except for mixed gonadal dysgenesis identified by karyotype alone. Treatment is ideal in a multidisciplinary setting with considerations to genetic (implications to family and reproductive recurrence risk), psychological aspects (sensitive individualized counseling including patient gender identity and preference), endocrinological (hormone replacement), surgical (cosmetic, prophylactic gonadectomy) fertility preservation and reproductive opportunities and metabolic health (cardiovascular and bones).

Publisher

Bioscientifica

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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