4.5 Article

Allelic overload and its clinical modifier effect in Bardet-Biedl syndrome

NPJ GENOMIC MEDICINE (2022)

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Journal

NPJ GENOMIC MEDICINE
Volume 7, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41525-022-00311-2

Keywords

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Categories

Genetics & Heredity

Funding

  1. Instituto de Salud Carlos III (ISCIII) of the Spanish Ministry of Health (FIS) [PI15/00049, PI16/00425, PI19/00321, PI19/00332]
  2. Centro de Investigacion Biomedica en Red Enfermedades Raras (CIBERER) [06/07/0036]
  3. IIS-FJD BioBank [PT13/0010/0012]
  4. Comunidad de Madrid (CAM, RAREGenomics Project) [B2017/BMD-3721]
  5. Xunta de Galicia (Centro de Investigacion de Galicia CINBIO 2019-2022) [ED431G-2019/06]
  6. Consolidacion e estructuracion de unidades de investigacion competitivas e outras accions de fomento (Xunta de Galicia) [ED431C-2018/54]
  7. European Regional Development Fund (FEDER)
  8. Organizacion Nacional de Ciegos Espanoles (ONCE)
  9. ISCIII [FI17/00192]
  10. Spanish Ministry of Education, Culture and Sports [FPU 19/00175]
  11. Miguel Servet program from ISCIII [CP16/00116]
  12. Fundacion Ramon Areces
  13. Fundacion Conchita Rabago
  14. University Chair UAM-IIS-FJD of Genomic Medicine

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This study aimed to investigate the role of mutational load in the clinical variability of Bardet-Biedl syndrome (BBS). Through clinical annotation and mutational load analysis, it was found that mutations in multiple BBS-associated genes may be associated with a more severe phenotype and specific clinical features. The study also revealed the potential role of oligogenic inheritance in BBS.
Bardet-Biedl syndrome (BBS) is an autosomal recessive ciliopathy characterized by extensive inter- and intra-familial variability, in which oligogenic interactions have been also reported. Our main goal is to elucidate the role of mutational load in the clinical variability of BBS. A cohort of 99 patients from 77 different families with biallelic pathogenic variants in a BBS-associated gene was retrospectively recruited. Human Phenotype Ontology terms were used in the annotation of clinical symptoms. The mutational load in 39 BBS-related genes was studied in index cases using different molecular and next-generation sequencing (NGS) approaches. Candidate allele combinations were analysed using the in silico tools ORVAL and DiGePred. After clinical annotation, 76 out of the 99 cases a priori fulfilled established criteria for diagnosis of BBS or BBS-like. BBS1 alleles, found in 42% of families, were the most represented in our cohort. An increased mutational load was excluded in 41% of the index cases (22/54). Oligogenic inheritance was suspected in 52% of the screened families (23/45), being 40 tested by means of NGS data and 5 only by traditional methods. Together, ORVAL and DiGePred platforms predicted an oligogenic effect in 44% of the triallelic families (10/23). Intrafamilial variable severity could be clinically confirmed in six of the families. Our findings show that the presence of more than two alleles in BBS-associated genes correlated in six families with a more severe phenotype and associated with specific findings, highlighting the role of the mutational load in the management of BBS cases.

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