Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families: Counseling and therapeutic implications

Purvi Majethia; Namanpreet Kaur; Selinda Mascarenhas; Lakshmi Priya Rao; Shruti Pande; Dhanya Lakshmi Narayanan; Vivekananda Bhat; Shalini S. Nayak; Karthik Vijay Nair; Adarsh Pooradan Prasannakumar; Ankur Chaurasia; Bhagesh Hunakunti; Nalesh Jadhav; Sheeba Farooqui; Mayuri Yeole; Vishaka Kothiwale; Rohit Naik; Veena Bhat; Shrikiran Aroor; Leslie Lewis; Jayashree Purkayastha; Y. Ramesh Bhat; B. K. Praveen; B. L. Yatheesha; Siddaramappa J. Patil; Sheela Nampoothiri; Nutan Kamath; Shahyan Siddiqui; Stephanie Bielas; Katta Mohan Girisha; Suvasini Sharma; Anju Shukla

doi:10.1111/cge.14495

Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families: Counseling and therapeutic implications

Purvi Majethia
, Namanpreet Kaur
, Selinda Mascarenhas
, Lakshmi Priya Rao
, Shruti Pande
, Dhanya Lakshmi Narayanan
, Vivekananda Bhat
, Shalini S. Nayak
, Karthik Vijay Nair
, Adarsh Pooradan Prasannakumar
, Ankur Chaurasia
, Bhagesh Hunakunti
, Nalesh Jadhav
, Sheeba Farooqui
, Mayuri Yeole
, Vishaka Kothiwale
, Rohit Naik
, Veena Bhat
, Shrikiran Aroor
, Leslie Lewis

Jayashree Purkayastha, Y. Ramesh Bhat, B. K. Praveen, B. L. Yatheesha, Siddaramappa J. Patil, Sheela Nampoothiri, Nutan Kamath, Shahyan Siddiqui, Stephanie Bielas, Katta Mohan Girisha, Suvasini Sharma^*, Anju Shukla^*

^*Corresponding author for this work

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

5 Citations (Scopus)

Abstract

The application of genomic technologies has led to unraveling of the complex genetic landscape of disorders of epilepsy, gaining insights into their underlying disease mechanisms, aiding precision medicine, and providing informed genetic counseling. We herein present the phenotypic and genotypic insights from 142 Indian families with epilepsy with or without comorbidities. Based on the electroclinical findings, epilepsy syndrome diagnosis could be made in 44% (63/142) of the families adopting the latest proposal for the classification by the ILAE task force (2022). Of these, 95% (60/63) of the families exhibited syndromes with developmental epileptic encephalopathy or progressive neurological deterioration. A definitive molecular diagnosis was achieved in 74 of 142 (52%) families. Infantile-onset epilepsy was noted in 81% of these families (61/74). Fifty-five monogenic, four chromosomal, and one imprinting disorder were identified in 74 families. The genetic variants included 65 (96%) single-nucleotide variants/small insertion-deletions, 1 (2%) copy-number variant, and 1 (2%) triplet-repeat expansion in 53 epilepsy-associated genes causing monogenic disorders. Of these, 35 (52%) variants were novel. Therapeutic implications were noted in 51% of families (38/74) with definitive diagnosis. Forty-one out of 66 families with monogenic disorders exhibited autosomal recessive and inherited autosomal dominant disorders with high risk of recurrence.

Original language	English
Pages (from-to)	639-654
Number of pages	16
Journal	Clinical Genetics
Volume	105
Issue number	6
DOIs	https://doi.org/10.1111/cge.14495
Publication status	Accepted/In press - 2024

All Science Journal Classification (ASJC) codes

Genetics
Genetics(clinical)

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10.1111/cge.14495

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Majethia, P., Kaur, N., Mascarenhas, S., Rao, L. P., Pande, S., Narayanan, D. L., Bhat, V., Nayak, S. S., Nair, K. V., Prasannakumar, A. P., Chaurasia, A., Hunakunti, B., Jadhav, N., Farooqui, S., Yeole, M., Kothiwale, V., Naik, R., Bhat, V., Aroor, S., ... Shukla, A. (Accepted/In press). Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families: Counseling and therapeutic implications. Clinical Genetics, 105(6), 639-654. https://doi.org/10.1111/cge.14495

@article{1c3757c6a9724a82a50356eebe478c30,

title = "Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families: Counseling and therapeutic implications",

abstract = "The application of genomic technologies has led to unraveling of the complex genetic landscape of disorders of epilepsy, gaining insights into their underlying disease mechanisms, aiding precision medicine, and providing informed genetic counseling. We herein present the phenotypic and genotypic insights from 142 Indian families with epilepsy with or without comorbidities. Based on the electroclinical findings, epilepsy syndrome diagnosis could be made in 44\% (63/142) of the families adopting the latest proposal for the classification by the ILAE task force (2022). Of these, 95\% (60/63) of the families exhibited syndromes with developmental epileptic encephalopathy or progressive neurological deterioration. A definitive molecular diagnosis was achieved in 74 of 142 (52\%) families. Infantile-onset epilepsy was noted in 81\% of these families (61/74). Fifty-five monogenic, four chromosomal, and one imprinting disorder were identified in 74 families. The genetic variants included 65 (96\%) single-nucleotide variants/small insertion-deletions, 1 (2\%) copy-number variant, and 1 (2\%) triplet-repeat expansion in 53 epilepsy-associated genes causing monogenic disorders. Of these, 35 (52\%) variants were novel. Therapeutic implications were noted in 51\% of families (38/74) with definitive diagnosis. Forty-one out of 66 families with monogenic disorders exhibited autosomal recessive and inherited autosomal dominant disorders with high risk of recurrence.",

author = "Purvi Majethia and Namanpreet Kaur and Selinda Mascarenhas and Rao, \{Lakshmi Priya\} and Shruti Pande and Narayanan, \{Dhanya Lakshmi\} and Vivekananda Bhat and Nayak, \{Shalini S.\} and Nair, \{Karthik Vijay\} and Prasannakumar, \{Adarsh Pooradan\} and Ankur Chaurasia and Bhagesh Hunakunti and Nalesh Jadhav and Sheeba Farooqui and Mayuri Yeole and Vishaka Kothiwale and Rohit Naik and Veena Bhat and Shrikiran Aroor and Leslie Lewis and Jayashree Purkayastha and Bhat, \{Y. Ramesh\} and Praveen, \{B. K.\} and Yatheesha, \{B. L.\} and Patil, \{Siddaramappa J.\} and Sheela Nampoothiri and Nutan Kamath and Shahyan Siddiqui and Stephanie Bielas and Girisha, \{Katta Mohan\} and Suvasini Sharma and Anju Shukla",

note = "Publisher Copyright: {\textcopyright} 2024 The Authors. Clinical Genetics published by John Wiley \& Sons Ltd.",

year = "2024",

doi = "10.1111/cge.14495",

language = "English",

volume = "105",

pages = "639--654",

journal = "Clinical Genetics",

issn = "0009-9163",

publisher = "Wiley-Blackwell Publishing Ltd",

number = "6",

}

Majethia, P, Kaur, N, Mascarenhas, S, Rao, LP, Pande, S, Narayanan, DL, Bhat, V , Nayak, SS, Nair, KV, Prasannakumar, AP, Chaurasia, A, Hunakunti, B, Jadhav, N, Farooqui, S, Yeole, M, Kothiwale, V, Naik, R, Bhat, V, Aroor, S , Lewis, L , Purkayastha, J, Bhat, YR, Praveen, BK, Yatheesha, BL, Patil, SJ, Nampoothiri, S, Kamath, N, Siddiqui, S, Bielas, S, Girisha, KM, Sharma, S & Shukla, A 2024, 'Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families: Counseling and therapeutic implications', Clinical Genetics, vol. 105, no. 6, pp. 639-654. https://doi.org/10.1111/cge.14495

TY - JOUR

T1 - Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families

T2 - Counseling and therapeutic implications

AU - Majethia, Purvi

AU - Kaur, Namanpreet

AU - Mascarenhas, Selinda

AU - Rao, Lakshmi Priya

AU - Pande, Shruti

AU - Narayanan, Dhanya Lakshmi

AU - Bhat, Vivekananda

AU - Nayak, Shalini S.

AU - Nair, Karthik Vijay

AU - Prasannakumar, Adarsh Pooradan

AU - Chaurasia, Ankur

AU - Hunakunti, Bhagesh

AU - Jadhav, Nalesh

AU - Farooqui, Sheeba

AU - Yeole, Mayuri

AU - Kothiwale, Vishaka

AU - Naik, Rohit

AU - Bhat, Veena

AU - Aroor, Shrikiran

AU - Lewis, Leslie

AU - Purkayastha, Jayashree

AU - Bhat, Y. Ramesh

AU - Praveen, B. K.

AU - Yatheesha, B. L.

AU - Patil, Siddaramappa J.

AU - Nampoothiri, Sheela

AU - Kamath, Nutan

AU - Siddiqui, Shahyan

AU - Bielas, Stephanie

AU - Girisha, Katta Mohan

AU - Sharma, Suvasini

AU - Shukla, Anju

PY - 2024

Y1 - 2024

N2 - The application of genomic technologies has led to unraveling of the complex genetic landscape of disorders of epilepsy, gaining insights into their underlying disease mechanisms, aiding precision medicine, and providing informed genetic counseling. We herein present the phenotypic and genotypic insights from 142 Indian families with epilepsy with or without comorbidities. Based on the electroclinical findings, epilepsy syndrome diagnosis could be made in 44% (63/142) of the families adopting the latest proposal for the classification by the ILAE task force (2022). Of these, 95% (60/63) of the families exhibited syndromes with developmental epileptic encephalopathy or progressive neurological deterioration. A definitive molecular diagnosis was achieved in 74 of 142 (52%) families. Infantile-onset epilepsy was noted in 81% of these families (61/74). Fifty-five monogenic, four chromosomal, and one imprinting disorder were identified in 74 families. The genetic variants included 65 (96%) single-nucleotide variants/small insertion-deletions, 1 (2%) copy-number variant, and 1 (2%) triplet-repeat expansion in 53 epilepsy-associated genes causing monogenic disorders. Of these, 35 (52%) variants were novel. Therapeutic implications were noted in 51% of families (38/74) with definitive diagnosis. Forty-one out of 66 families with monogenic disorders exhibited autosomal recessive and inherited autosomal dominant disorders with high risk of recurrence.

AB - The application of genomic technologies has led to unraveling of the complex genetic landscape of disorders of epilepsy, gaining insights into their underlying disease mechanisms, aiding precision medicine, and providing informed genetic counseling. We herein present the phenotypic and genotypic insights from 142 Indian families with epilepsy with or without comorbidities. Based on the electroclinical findings, epilepsy syndrome diagnosis could be made in 44% (63/142) of the families adopting the latest proposal for the classification by the ILAE task force (2022). Of these, 95% (60/63) of the families exhibited syndromes with developmental epileptic encephalopathy or progressive neurological deterioration. A definitive molecular diagnosis was achieved in 74 of 142 (52%) families. Infantile-onset epilepsy was noted in 81% of these families (61/74). Fifty-five monogenic, four chromosomal, and one imprinting disorder were identified in 74 families. The genetic variants included 65 (96%) single-nucleotide variants/small insertion-deletions, 1 (2%) copy-number variant, and 1 (2%) triplet-repeat expansion in 53 epilepsy-associated genes causing monogenic disorders. Of these, 35 (52%) variants were novel. Therapeutic implications were noted in 51% of families (38/74) with definitive diagnosis. Forty-one out of 66 families with monogenic disorders exhibited autosomal recessive and inherited autosomal dominant disorders with high risk of recurrence.

UR - https://www.scopus.com/pages/publications/85185651887

UR - https://www.scopus.com/pages/publications/85185651887#tab=citedBy

U2 - 10.1111/cge.14495

DO - 10.1111/cge.14495

M3 - Article

C2 - 38374498

AN - SCOPUS:85185651887

SN - 0009-9163

VL - 105

SP - 639

EP - 654

JO - Clinical Genetics

JF - Clinical Genetics

IS - 6

ER -

Genetic and phenotypic landscape of pediatric-onset epilepsy in 142 Indian families: Counseling and therapeutic implications

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