Molecular Diagnoses of X-Linked and Other Genetic Hypophosphatemias: Results From a Sponsored Genetic Testing Program

Rush, Eric T.; Johnson, Britt; Aradhya, Swaroop; Beltrán, Daniel; Bristow, Sara L.; Eisenbeis, Scott; Guerra, Norma; Krolczyk, Stan; Miller, Nicole L.; Morales, Ana; Ramesan, Prameela; Sarafrazi, Soodabeh; Truty, Rebecca; Dahir, Kathryn

doi:10.1002/jbmr.4454

Cited by 22 publications

(29 citation statements)

References 110 publications

(168 reference statements)

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“…ClinVar reports 814 XLH‐related variants in PHEX (accessed May 24, 2021), a recently updated count which includes 287 variants identified in the hypophosphatemia genetic testing program and reported to ClinVar (Rush et al, 2021 ). The locus‐specific database contributes another 50 novel XLH‐related PHEX variants which are presented here for the first time (Table S2 ).…”

Section: Resultsmentioning

confidence: 99%

“…The most prevalent variant in the database is a c.*231A>G substitution in the 3′‐UTR, which was frequently reported co‐occurring with an exon 13–15 duplication, suggesting that these two variants co‐segregate and constitute a single allele. In an analysis reported from the hypophosphatemia gene panel program, these variants were found together in both males and females in 65 of 66 probands and were shown to be in cis in all 51 individuals for whom phasing information was available (Rush et al, 2021 ).…”

Section: Resultsmentioning

confidence: 99%

“…Although the overall pattern of variants is consistent with previous studies, there has been a large increase in the number of CNV reported, which is likely a reflection of improved genetic testing methods for CNV. In the hypophosphatemia genetic testing program, 81% of the CNV events detected were sub‐genic and would be missed by traditional microarray analysis (Rush et al, 2021 ). However, despite the increased detection of CNV from more recent reports, most of the routine clinical testing methods employed so far, including those used in the hypophosphatemia genetic testing program, cannot detect deep intronic variants or large structural variants with breakpoints outside of the PHEX coding region.…”

Section: Discussionmentioning

confidence: 99%

“…The database was developed by integrating PHEX variants from four different sources: (1) a now inactive McGill University PHEX locus‐specific database (Sabbagh et al, 2000 ), last updated April, 2017, (2) genetic testing results from burosumab clinical trials, (3) a comprehensive literature review, and (4) a sponsored hypophosphatemia genetic testing program initiated by Ultragenyx Pharmaceutical Inc. and Invitae Corporation, which provided no‐charge next‐generation sequencing with a multi‐gene panel to confirm a clinical XLH diagnosis or to aid diagnosis of suspected XLH or other genetic hypophosphatemia (Rush et al, 2021 ). The hypophosphatemia genetic testing program was designed to detect single nucleotide variants (SNV), small and large insertions/deletions (indels), sub‐genic structural variants, and exon‐level copy number variants (CNV).…”

Section: Methodsmentioning

confidence: 99%

“…A new locus‐specific database for PHEX gene variants, PHEX LSDB, was established to collect and disseminate information to the scientific community and affected families about disease‐causing PHEX variants ( https://www.rarediseasegenes.com/ ). The database compiles variants from four sources: an older, archived PHEX locus‐specific variants database (Sabbagh et al, 2000 ), variants identified in a recent hypophosphatemia genetic testing program (Rush et al, 2021 ), unpublished variants identified in previous XLH clinical studies, and previously published variants identified from a comprehensive literature review. The PHEX LSDB will be updated regularly with new information on PHEX variants as reported in the literature or submitted directly to the database website.…”

Section: Introductionmentioning

confidence: 99%

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Novel PHEX gene locus‐specific database: Comprehensive characterization of vast number of variants associated with X‐linked hypophosphatemia (XLH)

et al. 2021

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X‐linked hypophosphatemia (XLH), the most common form of hereditary hypophosphatemia, is caused by disrupting variants in the PHEX gene, located on the X chromosome. XLH is inherited in an X‐linked pattern with complete penetrance observed for both males and females. Patients experience lifelong symptoms resulting from chronic hypophosphatemia, including impaired bone mineralization, skeletal deformities, growth retardation, and diminished quality of life. This chronic condition requires life‐long management with disease‐specific therapies, which can improve patient outcomes especially when initiated early in life. To centralize and disseminate PHEX variant information, we have established a new PHEX gene locus‐specific database, PHEX LSDB. As of April 30, 2021, 870 unique PHEX variants, compiled from an older database of PHEX variants, a comprehensive literature search, a sponsored genetic testing program, and XLH clinical trials, are represented in the PHEX LSDB. This resource is publicly available on an interactive, searchable website (https://www.rarediseasegenes.com/), which includes a table of variants and associated data, graphical/tabular outputs of genotype‐phenotype analyses, and an online submission form for reporting new PHEX variants. The database will be updated regularly with new variants submitted on the website, identified in the published literature, or shared from genetic testing programs.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Novel PHEX gene locus‐specific database: Comprehensive characterization of vast number of variants associated with X‐linked hypophosphatemia (XLH)

et al. 2021

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Mutation update: Variants of the ENPP1 gene in pathologic calcification, hypophosphatemic rickets, and cutaneous hypopigmentation with punctate keratoderma

Ralph

Levine

Richard³

et al. 2022

Human Mutation

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ENPP1 encodes ENPP1, an ectonucleotidase catalyzing hydrolysis of ATP to AMP and inorganic pyrophosphate (PPi), and an endogenous plasma protein physiologically preventing ectopic calcification of connective tissues. Mutations in ENPP1 have been reported in association with a range of human genetic diseases. In this mutation update, we provide a comprehensive review of all the pathogenic variants, likely pathogenic variants, and variants of unknown significance in ENPP1 associated with three autosomal recessive disorders—generalized arterial calcification of infancy (GACI), autosomal recessive hypophosphatemic rickets type 2 (ARHR2), and pseudoxanthoma elasticum (PXE), as well as with a predominantly autosomal dominant disorder—Cole disease. The classification of all variants is determined using the latest ACMG guidelines. A total of 140 ENPP1 variants were curated consisting of 133 previously reported variants and seven novel variants, with missense variants being the most prevalent (70.0%, 98/140). While the pathogenic variants are widely distributed in the ENPP1 gene of patientsgen without apparent genotype–phenotype correlation, eight out of nine variants associated with Cole disease are confined to the somatomedin‐B‐like (SMB) domains critical for homo‐dimerization of the ENPP1 protein.

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X‐Linked Hypophosphatemia Caused by the Prevailing North American PHEX Variant c.*231A>G; Exon 13–15 Duplication Is Often Misdiagnosed as Ankylosing Spondylitis and Manifests in Both Men and Women

et al. 2022

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Inactivating mutations of the gene coding for phosphate‐regulating endopeptidase homolog X‐linked (PHEX) cause X‐linked hypophosphatemia (XLH). A novel PHEX variant, c.*231A>G; exon 13–15 duplication, has emerged as a common cause of XLH in North America, emphasizing the importance of delineating its clinical presentation. Here, a comprehensive description of a five‐generation American kindred of 22 treatment‐naïve individuals harboring the c.*231A>G; exon 13–15 duplication is provided. After XLH was diagnosed in the proposita, pro‐active family members used social media to facilitate a timely assessment of their medical history. Most had normal height and 50% were normophosphatemic. Thirteen had been given a diagnosis other than XLH, most commonly ankylosing spondylitis, and XLH was only established after genetic testing. The prevalent phenotypic characteristics of c.*231A>G; exon 13–15 duplication were disorders of dentition (68.2%), enthesopathies (54.5%), fractures/bone and joint conditions (50%), lower‐limb deformities (40.9%), hearing loss/tinnitus (40.9%), gait abnormalities (22.7%), kidney stones/nephrocalcinosis (18.2%), chest wall disorders (9.1%), and Chiari/skull malformation (4.5%). More affected males than females, respectively, had gait abnormalities (42.9% versus 13.3%), lower‐limb deformities (71.4% versus 26.7%), and enthesopathies (85.7% versus 40%). Single phenotypes, observed exclusively in females, occurred in 22.7% and multiple phenotypes in 77.3% of the cohort. However, as many as six characteristics could develop in either affected males or females. Our findings will improve diagnostic and monitoring protocols for XLH. © 2022 The Authors. JBMR Plus published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research.

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Molecular Diagnoses of X-Linked and Other Genetic Hypophosphatemias: Results From a Sponsored Genetic Testing Program

Cited by 22 publications

References 110 publications

Novel PHEX gene locus‐specific database: Comprehensive characterization of vast number of variants associated with X‐linked hypophosphatemia (XLH)

Novel PHEX gene locus‐specific database: Comprehensive characterization of vast number of variants associated with X‐linked hypophosphatemia (XLH)

Mutation update: Variants of the ENPP1 gene in pathologic calcification, hypophosphatemic rickets, and cutaneous hypopigmentation with punctate keratoderma

X‐Linked Hypophosphatemia Caused by the Prevailing North American PHEX Variant c.*231A>G; Exon 13–15 Duplication Is Often Misdiagnosed as Ankylosing Spondylitis and Manifests in Both Men and Women

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