The Comprehensive Genetic Test for Abnormal Genitalia and Disorders of Sex Development (DSD) utilizes next-generation sequencing (NGS) to examine 73 genes associated with disorders of sex development and genital anomalies. It is a targeted gene panel specifically designed to support accurate diagnosis, risk assessment, and prevention.
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The Comprehensive Genetic Test for Abnormal Genitalia and Disorders of Sex Development (DSD) is a genetic test designed to identify mutations associated with a wide spectrum of congenital conditions affecting reproductive system development. This panel analyzes a curated set of genes responsible for disorders of sex development, enabling precise diagnosis, determination of chromosomal and gonadal sex, and guidance for clinical management and long-term care planning.
Disorders of sex development are a heterogeneous group of conditions characterized by discrepancies between chromosomal, gonadal, and anatomical sex. These conditions may manifest as ambiguous genitalia at birth, atypical development of internal or external reproductive structures, or discrepancies in pubertal progression. Disorders of sex development (DSDs) can occur in individuals with a typical 46,XX or 46,XY karyotype, as well as in those with sex chromosome mosaicism or structural abnormalities. The genetic causes are diverse, involving genes that regulate gonadal differentiation, steroid hormone biosynthesis, androgen action, and the development of reproductive structures.
The Comprehensive Genetic Test for Abnormal Genitalia and Disorders of Sex Development (DSD) evaluates key genes, including SRY, NR5A1 (SF1), SOX9, AR, CYP21A2, WT1, FOXL2, and AMH. These genes influence pathways critical for sex determination, gonadal formation, adrenal function, and genital development. The test is indicated in cases of ambiguous genitalia, primary amenorrhea, atypical pubertal development, or when imaging reveals discordant internal reproductive anatomy. It is also appropriate for individuals with a family history of disorders of sex development (DSDs) or unexplained infertility linked to underlying sexual differentiation defects.
The identification of a pathogenic variant confirms the molecular basis of the disorder and facilitates accurate classification and tailored treatment decisions, including considerations for hormone therapy, surgical management, and fertility preservation. Variants of uncertain significance may also be detected and require integration with clinical and endocrinological data. When no mutations are identified but clinical suspicion persists, further testing, including chromosomal analysis or expanded panels, may be warranted.
An increased genetic risk is identified when a known pathogenic mutation is present, especially in individuals with phenotypic-genotypic discrepancies or a family history of disorders of sex development (DSDs). A lower risk may be indicated when no relevant mutations are found, though residual risk remains due to potential limitations in testing sensitivity or uncharacterized genetic mechanisms. Comprehensive evaluation must always be based on clinical presentation, hormonal profiling, imaging, and family history, with results used to guide diagnostic clarification and multidisciplinary care.
The test is performed in a clinical laboratory accredited to ISO 15189 and certified by CLIA and CAP, ensuring the validity, accuracy and international recognition of the results.
