Clinical presentation and evolution of Xia‐Gibbs syndrome due to p.Gly375ArgfsTer3 variant in a patient from DR Congo (Central Africa)

Mubungu, Gerrye; Makay, Prince; Boujemla, Bouchra; Yanda, Stephane; Posey, Jennifer E.; Lupski, James R.; Lukusa, Prosper Tshilobo; Devriendt, Koenraad; Lumaka, Aimé

doi:10.1002/ajmg.a.62049

Cited by 11 publications

(9 citation statements)

References 9 publications

(14 reference statements)

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“…In a recent work by Khayat et al, truncating mutations closer to the N‐terminus were more likely associated with seizures or scoliosis (Khayat et al, 2021). However, phenotypic heterogeneity is not uncommon in individuals harboring the same variant, suggesting that clear‐cut genotype–phenotype correlations are difficult to establish (Jiang et al, 2018; Mubungu et al, 2020). In fact, two unrelated children carrying the c.2849del (p.Pro950Argfs*192) variant have been recently reported to show significantly different phenotypes (Faergeman et al, 2021).…”

Section: Discussionmentioning

confidence: 99%

Genotype–phenotype spectrum and correlations in Xia‐Gibbs syndrome: Report of five novel cases and literature review

Romano,

Falco,

Cappuccio

et al. 2022

Birth Defects Research

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Background: Xia-Gibbs syndrome (XGS) is a rare neurodevelopmental disorder caused by pathogenic variants in the AT-hook DNA-binding motif-containing 1 gene (AHDC1), encoding a protein with a crucial role in transcription and epigenetic regulation, axonogenesis, brain function, and neurodevelopment. AHDC1 variants possibly act through a dominant-negative mechanism and may interfere with DNA repair processes, leading to genome Dr Ferruccio Romano and Mariateresa Falco have contributed equally. Dr Marcello Scala and Dr Valeria Capra have contributed equally.

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Section: Discussionmentioning

confidence: 99%

Genotype–phenotype spectrum and correlations in Xia‐Gibbs syndrome: Report of five novel cases and literature review

Romano,

Falco,

Cappuccio

et al. 2022

Birth Defects Research

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“…gov/ clinv ar/), against a good population database illustrated enrichment of ClinVar with a significant proportion of wrongly ascertained variants [27]. Also, reanalysis of NGS data after databases have been populated helped in both identifying previously discarded plausible variants and down-classifying previously misclassified variants [28][29][30][31]. Such misclassification was found to be higher in individuals of African ancestry [32].…”

Section: Challenges Facing Africa For Resolution Of Rare Undiagnosed ...mentioning

confidence: 99%

“…In addition, there is an important contribution of NGS tests free-of-charge to African rare diseases patients from international research collaborations and philanthropic initiatives such as the Centers for Mendelian Genomics (CMG) [12] and the iHope foundation. All these efforts have allowed ending diagnostic odyssey in many African patients and adjusting care when possible as well as identifying new disease genes [13][14][15][16][17][18].…”

Section: Contextmentioning

confidence: 99%

“…The first consequence of the underrepresentation of African samples from commonly used databases is the higher level of difficulty to reach a molecular diagnosis in African individuals. The data disparity ultimately results in health disparity [17]. There is a risk that NGS will be perceived as deeply flawed and thus of limited clinical utility for some populations, which would work against all of the efforts to make this technology more accessible on the African continent.…”

Section: Challenges Facing Africa For Resolution Of Rare Undiagnosed ...mentioning

confidence: 99%

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Increasing African genomic data generation and sharing to resolve rare and undiagnosed diseases in Africa: a call-to-action by the H3Africa rare diseases working group

Lumaka

Carstens

Devriendt

et al. 2022

Orphanet J Rare Dis

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The rich and diverse genomics of African populations is significantly underrepresented in reference and in disease-associated databases. This renders interpreting the Next Generation Sequencing (NGS) data and reaching a diagnostic more difficult in Africa and for the African diaspora. It increases chances for false positives with variants being misclassified as pathogenic due to their novelty or rarity. We can increase African genomic data by (1) making consent for sharing aggregate frequency data an essential component of research toolkit; (2) encouraging investigators with African data to share available data through public resources such as gnomAD, AVGD, ClinVar, DECIPHER and to use MatchMaker Exchange; (3) educating African research participants on the meaning and value of sharing aggregate frequency data; and (4) increasing funding to scale-up the production of African genomic data that will be more representative of the geographical and ethno-linguistic variation on the continent. The RDWG of H3Africa is hereby calling to action because this underrepresentation accentuates the health disparities. Applying the NGS to shorten the diagnostic odyssey or to guide therapeutic options for rare diseases will fully work for Africans only when public repositories include sufficient data from African subjects.

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“…and overlaps with other disorders, making it challenging to diagnose based on clinical presentation alone. All reported diagnoses have so far been established by DNA sequence-based approaches (Cardosodos-Santos et al, 2020;Cheng et al, 2019;Díaz-Ordoñez et al, 2019;García-Acero & Acosta, 2017;Gumus, 2020;He et al, 2020;Jiang et al, 2018;Mubungu et al, 2020;Murdock et al, 2019;Ritter et al, 2018;Xia et al, 2014;H. Yang et al, 2015;S.…”

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confidence: 99%

Phenotypic and protein localization heterogeneity associated with AHDC1 pathogenic protein‐truncating alleles in Xia–Gibbs syndrome

Khayat

Chander

et al. 2021

Human Mutation

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Xia-Gibbs syndrome (XGS) is a rare Mendelian disease typically caused by de novo stop-gain or frameshift mutations in the AT-hook DNA binding motif containing 1 (AHDC1) gene. Patients usually present in early infancy with hypotonia and developmental delay and later exhibit intellectual disability (ID). The overall presentation is variable, however, and the emerging clinical picture is still evolving. A detailed phenotypic analysis of 34 XGS individuals revealed five core phenotypes (delayed motor milestones, speech delay, low muscle tone, ID, and hypotonia) in more than 80% of individuals and an additional 12 features that occurred more variably.Seizures and scoliosis were more frequently associated with truncations that arise before the midpoint of the protein although the occurrence of most features could not be predicted by the mutation position. Transient expression of wild type and different patient truncated AHDC1 protein forms in human cell lines revealed abnormal patterns of nuclear localization including a diffuse distribution of a short truncated form and nucleolar aggregation in mid-protein truncated forms. Overall, both the occurrence of variable phenotypes and the different distribution of the expressed protein reflect the heterogeneity of this syndrome.

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Clinical presentation and evolution of Xia‐Gibbs syndrome due to p.Gly375ArgfsTer3 variant in a patient from DR Congo (Central Africa)

Cited by 11 publications

References 9 publications

Genotype–phenotype spectrum and correlations in Xia‐Gibbs syndrome: Report of five novel cases and literature review

Genotype–phenotype spectrum and correlations in Xia‐Gibbs syndrome: Report of five novel cases and literature review

Increasing African genomic data generation and sharing to resolve rare and undiagnosed diseases in Africa: a call-to-action by the H3Africa rare diseases working group

Phenotypic and protein localization heterogeneity associated with AHDC1 pathogenic protein‐truncating alleles in Xia–Gibbs syndrome

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