Integrated small copy number variations and epigenome maps of disorders of sex development

Amarillo, Ina; Nievera, Isabelle; Hagan, Andrew; Huchthagowder, Vishwa; Heeley, Jennifer; Hollander, Abby; Koenig, Joel F.; Austin, Paul F.; Wang, Ting

doi:10.1038/hgv.2016.12

Cited by 22 publications

(29 citation statements)

References 65 publications

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“…5,27–30 Genome-wide maps of CNVs of known pathogenicity as well as of uncertain clinical significance will continue to support clinical diagnosis and drive research for new etiologies. 31 The advent of next-generation sequencing in the realm of clinical diagnosis in the past 4 to 5 years is now allowing providers to rethink the diagnostic process.…”

Section: Improve and Accelerate The Path To An Accurate Diagnosis Formentioning

confidence: 99%

Genetics of Disorders of Sex Development

Sandberg¹,

Délot

Fox³

et al. 2017

Endocrinology and Metabolism Clinics of North America

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The Disorders of Sex Development (DSD) Consensus Conference, held in Chicago in 2005, identified several domains of care where improvement was needed.1 In particular, it called for the establishment of an infrastructure for collaborative interdisciplinary clinical practice and research, with the goal of integrating scientific understanding of DSD with real-time standardization and improvement in clinical practice. The DSD-Translational Research Network (DSD-TRN) was created in response, the first such North American infrastructure, a network of 4 (now expanded to 10) research and clinical sites and a central registry, with the collaboration of Accord Alliance, a nonprofit convener of diverse DSD stakeholders. To address the variability within and across medical, surgical, and behavioral health aspects of care, the DSD-TRN is dedicated to the standardization of diagnostic and treatment protocols in order to enhance clinical and scientific discovery, as well as quality of life outcomes for patients and their families. A critical aspect of this standardization of practice is a commitment to an early and comprehensive diagnostic process (including genetic), associated with extensive standardized phenotyping and psychosocial screening and support of patients and families. A recent review of the state of clinical, biochemical, genetic, and psychosocial evaluations of the newborn or adolescent with DSD, 10 years after the consensus statement, continued to highlight the need for a thorough diagnostic process that sets in motion informed discussions with parents (and newly diagnosed adolescent patients) regarding treatment options.2 Developmental pathways of sex determination and differentiation impacted in isolated and syndromic DSD conditions were recently reviewed.3–5 This article will briefly review the main categories of genetic causes of DSD and the diagnostic revolution promised by the advent of new genomic technology, and will present the DSD-TRN guidelines for genetic diagnosis, features of the registry for future research, and a peek into some early registry data.

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Section: Improve and Accelerate The Path To An Accurate Diagnosis Formentioning

confidence: 99%

Genetics of Disorders of Sex Development

Sandberg¹,

Délot

Fox³

et al. 2017

Endocrinology and Metabolism Clinics of North America

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“…Another large cohort of eighty‐seven 46,XY GD patients was screened with a diagnostic hit rate of 30% (Ledig et al, ), while a smaller screen of 46,XY DSD patients found CNVs in 23.8% of cases by jointly utilizing a CGH microarray, as well as Multiplex ligation‐dependant Probe Amplification (MPLA) for validation (White et al, ). More recently these technologies have been combined with epigenomic studies using a retrospective analysis to create a high‐density gene specific CNV and epigenomic maps from patients with DSD, in an effort to improve the diagnostic potential of CNV screening (Amarillo et al, ).…”

Section: Dsd Gene Discovery and Screening For Causative Mutationsmentioning

confidence: 99%

Corrigendum: Corrigendum for: Disorders of sex development: The evolving role of genomics in diagnosis and gene discovery, 108:337–350 (10.1002/bdrc.21148)

Croft¹,

Ayers²,

Sinclair³

et al. 2017

Birth Defects Research

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Disorders of Sex Development (DSDs) are a major paediatric concern and are estimated to occur in around 1.7% of all live births (Fausto‐Sterling, Sexing the Body: Gender Politics and the Construction of Sexuality, Basic Books, New York, 2000). They are often caused by the breakdown in the complex genetic mechanisms that underlie gonadal development and differentiation. Having a genetic diagnosis can be important for patients with a DSD: it can increase acceptance of a disorder often surrounded by stigma, alter clinical management and it can assist in reproductive planning. While Massively Parallel Sequencing (MPS) is advancing the genetic diagnosis of rare Mendelian disorders, it is not yet clear which MPS assay is best suited for the clinical diagnosis of DSD patients and to what extent other established methods are still relevant. To complicate matters, DSDs represent a wide spectrum of disorders caused by an array of different genetic changes, many of which are yet unknown. Here we discuss the different genetic lesions that are known to contribute to different DSDs, and review the utility of a range of MPS approaches for diagnosing DSD patients. Birth Defects Research (Part C) 108:337–350, 2016. © 2016 Wiley Periodicals, Inc.

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“…NGS-based techniques have also now made their appearance in prenatal diagnosis of congenital anomalies 29 30. Panels using these techniques can be specific for genes involved in DSD, or be larger panels covering multiple congenital anomalies, and are usually employed with trio-analysis to compare variants identified in the child with the parents’ genetics 29–31. Finding a genetic cause before delivery can help reduce parental stress in the neonatal period and speed up decisions regarding gender assignment.…”

Section: Guideline Highlightsmentioning

confidence: 99%

“…Very recently, a European position paper has been published focusing on the genetic workup of DSD 16. It highlights the limitations and drawbacks of NGS-based tests, which include the chance of missing subtle structural variants such as CNVs and mosaicism and the fact that NGS cannot detect methylation defects or other epigenetic changes 16 28 31. Targeted DNA analysis is preferred in cases where hormonal investigations suggest a block in steroidogenesis (eg, 11-β-hydroxylase deficiency, 21-hydroxylase deficiency), or in the context of a specific clinical constellation such as the often coincidental finding of Müllerian structures in a boy with normal external genitalia or cryptorchidism, that is, persistent Müllerian duct syndrome 33 34.…”

Section: Guideline Highlightsmentioning

confidence: 99%