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

Dhanya Lakshmi Narayanan; Divya Udyawar; Parneet Kaur; Suvasini Sharma; Narayanaswamy Suresh; Sheela Nampoothiri; Michelle C. do Rosario; Puneeth H. Somashekar; Lakshmi Priya Rao; Neethukrishna Kausthubham; Purvi Majethia; Shruti Pande; Y. Ramesh Bhat; Aroor Shrikiran; Stephanie Bielas; Katta Mohan Girisha; Anju Shukla

doi:10.1038/s41431-021-00933-7

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

Dhanya Lakshmi Narayanan
, Divya Udyawar
, Parneet Kaur
, Suvasini Sharma
, Narayanaswamy Suresh
, Sheela Nampoothiri
, Michelle C. do Rosario
, Puneeth H. Somashekar
, Lakshmi Priya Rao
, Neethukrishna Kausthubham
, Purvi Majethia
, Shruti Pande
, Y. Ramesh Bhat
, Aroor Shrikiran
, Stephanie Bielas
, Katta Mohan Girisha
, Anju Shukla^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

18 Citations (Scopus)

Abstract

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.

Original language	English
Pages (from-to)	1774-1780
Number of pages	7
Journal	European Journal of Human Genetics
Volume	29
Issue number	12
DOIs	https://doi.org/10.1038/s41431-021-00933-7
Publication status	Published - 12-2021

All Science Journal Classification (ASJC) codes

Genetics
Genetics(clinical)

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Narayanan, D. L., Udyawar, D., Kaur, P., Sharma, S., Suresh, N., Nampoothiri, S., do Rosario, M. C., Somashekar, P. H., Rao, L. P., Kausthubham, N., Majethia, P., Pande, S., Ramesh Bhat, Y., Shrikiran, A., Bielas, S., Girisha, K. M., & Shukla, A. (2021). Multilocus disease-causing genomic variations for Mendelian disorders: role of systematic phenotyping and implications on genetic counselling. European Journal of Human Genetics, 29(12), 1774-1780. https://doi.org/10.1038/s41431-021-00933-7

@article{d93f438c91d346ed9cfcf3bc3eb5f1c5,

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

abstract = "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.",

author = "Narayanan, \{Dhanya Lakshmi\} and Divya Udyawar and Parneet Kaur and Suvasini Sharma and Narayanaswamy Suresh and Sheela Nampoothiri and \{do Rosario\}, \{Michelle C.\} and Somashekar, \{Puneeth H.\} and Rao, \{Lakshmi Priya\} and Neethukrishna Kausthubham and Purvi Majethia and Shruti Pande and \{Ramesh Bhat\}, Y. and Aroor Shrikiran and Stephanie Bielas and Girisha, \{Katta Mohan\} and Anju Shukla",

note = "Funding Information: This study was conducted with the support of the funding received from the following research projects: 1. “Genetic Diagnosis of Neurodevelopmental Disorders in India” (1R01HD093570-01A1) funded by the National Institutes of Health, United States. 2. “Clinical and molecular characterisation of leukodystrophies in Indian children” (V.25011/379/2015-GIA/HR) funded by the Department of Health Research, Government of India. 3. Science and Engineering Research Board, Government of India (YSS/2015/002009). Open access funding provided by Manipal Academy of Higher Education, Manipal. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = dec,

doi = "10.1038/s41431-021-00933-7",

language = "English",

volume = "29",

pages = "1774--1780",

journal = "European Journal of Human Genetics",

issn = "1018-4813",

publisher = "Springer Nature",

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Narayanan, DL, Udyawar, D, Kaur, P, Sharma, S, Suresh, N, Nampoothiri, S, do Rosario, MC, Somashekar, PH, Rao, LP, Kausthubham, N, Majethia, P, Pande, S, Ramesh Bhat, Y , Shrikiran, A, Bielas, S, Girisha, KM & Shukla, A 2021, 'Multilocus disease-causing genomic variations for Mendelian disorders: role of systematic phenotyping and implications on genetic counselling', European Journal of Human Genetics, vol. 29, no. 12, pp. 1774-1780. https://doi.org/10.1038/s41431-021-00933-7

TY - JOUR

T1 - Multilocus disease-causing genomic variations for Mendelian disorders

T2 - role of systematic phenotyping and implications on genetic counselling

AU - Narayanan, Dhanya Lakshmi

AU - Udyawar, Divya

AU - Kaur, Parneet

AU - Sharma, Suvasini

AU - Suresh, Narayanaswamy

AU - Nampoothiri, Sheela

AU - do Rosario, Michelle C.

AU - Somashekar, Puneeth H.

AU - Rao, Lakshmi Priya

AU - Kausthubham, Neethukrishna

AU - Majethia, Purvi

AU - Pande, Shruti

AU - Ramesh Bhat, Y.

AU - Shrikiran, Aroor

AU - Bielas, Stephanie

AU - Girisha, Katta Mohan

AU - Shukla, Anju

N1 - Funding Information: This study was conducted with the support of the funding received from the following research projects: 1. “Genetic Diagnosis of Neurodevelopmental Disorders in India” (1R01HD093570-01A1) funded by the National Institutes of Health, United States. 2. “Clinical and molecular characterisation of leukodystrophies in Indian children” (V.25011/379/2015-GIA/HR) funded by the Department of Health Research, Government of India. 3. Science and Engineering Research Board, Government of India (YSS/2015/002009). Open access funding provided by Manipal Academy of Higher Education, Manipal. Publisher Copyright: © 2021, The Author(s).

PY - 2021/12

Y1 - 2021/12

N2 - 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.

AB - 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.

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UR - https://www.scopus.com/pages/publications/85110644517#tab=citedBy

U2 - 10.1038/s41431-021-00933-7

DO - 10.1038/s41431-021-00933-7

M3 - Article

AN - SCOPUS:85110644517

SN - 1018-4813

VL - 29

SP - 1774

EP - 1780

JO - European Journal of Human Genetics

JF - European Journal of Human Genetics

IS - 12

ER -

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

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