Multilocus disease-causing genomic variations for Mendelian disorders: role of systematic phenotyping and implications on genetic counselling

Multilocus disease-causing genomic variations (MGVs) and multiple genetic diagnoses (MGDs) are increasingly being recognised in individuals and families with Mendelian disorders. This can be mainly attributed to the widespread use of genomic tests for the evaluation of these disorders. We conducted...

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Bibliographic Details
Published in:European journal of human genetics : EJHG 2021-12, Vol.29 (12), p.1774-1780
Main Authors: Narayanan, Dhanya Lakshmi, Udyawar, Divya, Kaur, Parneet, Sharma, Suvasini, Suresh, Narayanaswamy, Nampoothiri, Sheela, do Rosario, Michelle C, Somashekar, Puneeth H, Rao, Lakshmi Priya, Kausthubham, Neethukrishna, Majethia, Purvi, Pande, Shruti, Ramesh Bhat, Y, Shrikiran, Aroor, Bielas, Stephanie, Girisha, Katta Mohan, Shukla, Anju
Format: Article
Language:English
Subjects:
Age
Consanguinity
Counseling
Families & family life
Female
Genetic counseling
Genetic Counseling - methods
Genetic Diseases, Inborn - diagnosis
Genetic Diseases, Inborn - genetics
Genetic diversity
Genetic Testing - methods
Genetics
Genomes
Genomics
Genotype & phenotype
Higher education
Humans
Inbreeding
Male
Medical schools
Multifactorial Inheritance
Pediatrics
Pedigree
Penetrance
Phenotypes
Phenotyping
Polymorphism, Genetic
Quantitative Trait Loci
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Summary:Multilocus disease-causing genomic variations (MGVs) and multiple genetic diagnoses (MGDs) are increasingly being recognised in individuals and families with Mendelian disorders. This can be mainly attributed to the widespread use of genomic tests for the evaluation of these disorders. We conducted a retrospective study of families evaluated over the last 6 years at our centre to identify families with MGVs and MGDs. MGVs were observed in fourteen families. We observed five different consequences: (i) individuals with MGVs presenting as blended phenotypes (ii) individuals with MGVs presenting with distinct phenotypes (iii) individuals with MGVs with age-dependent penetrance (iv) individuals with MGVs with one phenotype obscured by another more predominant phenotype (v) two distinct phenotypes in different individuals in families with MGVs. Consanguinity was present in eight (8/14, 57.1%) of them. Thirteen families had two Mendelian disorders and one had three Mendelian disorders. The risk of recurrence of one or more conditions in these families ranged from 25% to 75%. Our findings underline the importance of the role of a clinical geneticist in systematic phenotyping, challenges in genetic counselling and risk estimation in families with MGVs and MGDs, especially in highly inbred populations.
ISSN:1018-4813
1476-5438
DOI:10.1038/s41431-021-00933-7