Case-control association study of congenital heart disease from a tertiary paediatric cardiac centre from North India

Prachi Kukshal; Radha O Joshi; Ajay Kumar; Shadab Ahamad; Prabhatha Rashmi Murthy; Yogesh Sathe; Krishna Manohar; Soma Guhathakurta; Subramanian Chellappan

doi:10.1186/s12887-023-04095-x

Case-control association study of congenital heart disease from a tertiary paediatric cardiac centre from North India

BMC Pediatr. 2023 Jun 15;23(1):290. doi: 10.1186/s12887-023-04095-x.

Authors

Prachi Kukshal¹, Radha O Joshi², Ajay Kumar³, Shadab Ahamad³, Prabhatha Rashmi Murthy⁴, Yogesh Sathe⁵, Krishna Manohar⁵, Soma Guhathakurta³, Subramanian Chellappan⁶

Affiliations

¹ Sri Sathya Sai Sanjeevani Research Foundation, NH-2, Delhi-Mathura Highway, Baghola, Haryana, District Palwal, Pin- 121102, India. prachi7k@gmail.com.
² Present address Sri Sathya Sai Sanjeevani Research Foundation, Kharghar, Navi Mumbai- 410210, Maharashtra, India.
³ Sri Sathya Sai Sanjeevani Research Foundation, NH-2, Delhi-Mathura Highway, Baghola, Haryana, District Palwal, Pin- 121102, India.
⁴ Sri Sathya Sai Sanjeevani Centre for Child Heart Care and Training in Paediatric Cardiac Skills, Navi Mumbai Maharashtra, India.
⁵ Sri Sathya Sai Sanjeevani International Centre for Child Heart Care & Research, NH-2, Delhi-Mathura Highway, Baghola, District Palwal, Haryana, Pin 121102, India.
⁶ Sri Sathya Sai Sanjeevani International Centre for Child Heart Care & Research, NH-2, Delhi-Mathura Highway, Baghola, District Palwal, Haryana, Pin 121102, India. subramanianchellappan@gmail.com.

Abstract

Background: Congenital Heart diseases (CHDs) account for 1/3rd of all congenital birth defects. Etiopathogenesis of CHDs remain elusive despite extensive investigations globally. Phenotypic heterogeneity witnessed in this developmental disorder reiterate gene-environment interactions with periconceptional factors as risk conferring; and genetic analysis of both sporadic and familial forms of CHD suggest its multigenic basis. Significant association of de novo and inherited variants have been observed. Approximately 1/5th of CHDs are documented in the ethnically distinct Indian population but genetic insights have been very limited. This pilot case-control based association study was undertaken to investigate the status of Caucasian SNPs in a north Indian cohort.

Method: A total of 306 CHD cases sub-classified into n = 198 acyanotic and n = 108 cyanotic types were recruited from a dedicated tertiary paediatric cardiac centre in Palwal, Haryana. 23 SNPs primarily prioritized from Genome-wide association studies (GWAS) on Caucasians were genotyped using Agena MassARRAY Technology and test of association was performed with adequately numbered controls.

Results: Fifty percent of the studied SNPs were substantially associated in either allelic, genotypic or sub-phenotype categories validating their strong correlation with disease manifestation. Of note, strongest allelic association was observed for rs73118372 in CRELD1 (p < 0.0001) on Chr3, rs28711516 in MYH6 (p = 0.00083) and rs735712 in MYH7 (p = 0.0009) both on Chr 14 and were also significantly associated with acyanotic, and cyanotic categories separately. rs28711516 (p = 0.003) and rs735712 (p = 0.002) also showed genotypic association. Strongest association was observed with rs735712(p = 0.003) in VSD and maximum association was observed for ASD sub-phenotypes.

Conclusions: Caucasian findings were partly replicated in the north Indian population. The findings suggest the contribution of genetic, environmental and sociodemographic factors, warranting continued investigations in this study population.

Keywords: Case–control association; Congenital Heart Disease; GWAS variants; North India.

MeSH terms

Case-Control Studies
Genome-Wide Association Study*
Genotype
Heart Defects, Congenital* / complications
Heart Defects, Congenital* / epidemiology
Heart Defects, Congenital* / genetics
Humans
India / epidemiology
White People / genetics