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Burden of rare genetic disorders in India: twenty-two years' experience of a tertiary centre.
Sheth, Jayesh; Nair, Aadhira; Sheth, Frenny; Ajagekar, Manali; Dhondekar, Tejasvi; Panigrahi, Inusha; Bavdekar, Ashish; Nampoothiri, Sheela; Datar, Chaitanya; Gandhi, Ajit; Muranjan, Mamta; Kaur, Anupriya; Desai, Manisha; Mistri, Mehul; Patel, Chitra; Naik, Premal; Shah, Maulin; Godbole, Koumudi; Kapoor, Seema; Gupta, Neerja; Bijarnia-Mahay, Sunita; Kadam, Sandeep; Solanki, Dhaval; Desai, Soham; Iyer, Anand; Patel, Ketan; Patel, Harsh; Shah, Raju C; Mehta, Shalmi; Shah, Ruchi; Bhavsar, Riddhi; Shah, Jhanvi; Pandya, Mili; Patel, Bhagyadhan; Shah, Sudhir; Shah, Heli; Shah, Shalin; Bajaj, Shruti; Shah, Siddharth; Thaker, Nilam; Kalane, Umesh; Kamate, Mahesh; Kn, Vykunta Raju; Tayade, Naresh; Jagadeesan, Sujatha; Jain, Deepika; Chandarana, Mitesh; Singh, Jitendra; Mehta, Sanjiv; Suresh, Beena.
Afiliação
  • Sheth J; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India. jayesh.sheth@frige.co.in.
  • Nair A; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Sheth F; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Ajagekar M; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Dhondekar T; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Panigrahi I; Postgraduate Institute of Medical Education and Research, PGIMER, Chandigarh, India.
  • Bavdekar A; Department of Pediatrics, K.E.M Hospital, Pune, India.
  • Nampoothiri S; Department of Paediatrics, Amrita School of Medicine, Kochi, India.
  • Datar C; Bharati Hospital and Research Centre, Dhankawadi, Pune, India.
  • Gandhi A; Unique Hospital, Solapur, India.
  • Muranjan M; Department of Pediatrics, KEM Hospital, Parel, Mumbai, India.
  • Kaur A; Postgraduate Institute of Medical Education and Research, PGIMER, Chandigarh, India.
  • Desai M; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Mistri M; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Patel C; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Naik P; Rainbow Super speciality Hospital, Ahmedabad, India.
  • Shah M; Ortho Kids Clinic, Ahmedabad, India.
  • Godbole K; Deenanath Mangeshkar Hospital & Research Centre, Pune, India.
  • Kapoor S; Division of Genetics & Metabolism Department of Pediatrics, Lok Nayak Hospital and Maulana Azad Medical College, New Delhi, India.
  • Gupta N; Division of Genetics, Department of Pediatrics, All India Institute of Medical Sciences, New Delhi, India.
  • Bijarnia-Mahay S; Institute of Medical Genetics and Genomics, Sir Ganga Ram Hospital, New Delhi, India.
  • Kadam S; Department of Pediatrics, K.E.M Hospital, Pune, India.
  • Solanki D; Nirmal Mantra Children's Hospital, Bhavnagar, India.
  • Desai S; Shree Krishna Hospital, Karamsad, Anand, India.
  • Iyer A; Neuro Kids Clinics, Ahmedabad, India.
  • Patel K; Himalaya Arcade, Homeopathy Clinic, Vastrapur, Ahmedabad, India.
  • Patel H; Zydus Hospital & Healthcare Research Pvt Ltd, Ahmedabad, India.
  • Shah RC; Ankur Neonatal Hospital, Ashram Road, Ahmedabad, India.
  • Mehta S; Endokids Clinic, Ahmedabad, India.
  • Shah R; Endokids Clinic, Ahmedabad, India.
  • Bhavsar R; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Shah J; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Pandya M; FRIGE Institute of Human Genetics, FRIGE House, Ahmedabad, India.
  • Patel B; Brain and Nerve Clinic, Sola, Ahmedabad, India.
  • Shah S; NHL Medical College, Ahmedabad, India.
  • Shah H; Ansa Clinic, S. G. Highway, Ahmedabad, India.
  • Shah S; Ansa Clinic, S. G. Highway, Ahmedabad, India.
  • Bajaj S; The Purple Gene Clinic, Simplex Khushaangan, SV Road, Malad West, Mumbai, India.
  • Shah S; RICN Hospital, Ahmedabad, India.
  • Thaker N; Pediatric Nephrologist, Ahmedabad, India.
  • Kalane U; Deenanath Mangeshkar Hospital & Research Centre, Pune, India.
  • Kamate M; KLES Prabhakar Kore Hospital, Belgaum, India.
  • Kn VR; Department of Pediatric Neurology, Indira Gandhi Institute of Child Health, Bangalore, India.
  • Tayade N; Department of Paediatrics, Dr. Panjabrao Deshmukh Memorial Medical College, Amravati, India.
  • Jagadeesan S; Department of Clinical Genetics & Genetic Counselling, Mediscan Systems, Chennai, India.
  • Jain D; Shishu Child Development and Early Intervention Centre, Ahmedabad, India.
  • Chandarana M; Medisquare Superspeciality Hospital and Research Institute, Ahmedabad, India.
  • Singh J; Neurology Clinic, Shivranjini Cross Road, Satellite, Ahmedabad, India.
  • Mehta S; RICN Hospital, Ahmedabad, India.
  • Suresh B; Department of Clinical Genetics & Genetic Counselling, Mediscan Systems, Chennai, India.
Orphanet J Rare Dis ; 19(1): 295, 2024 Aug 13.
Article em En | MEDLINE | ID: mdl-39138584
ABSTRACT

BACKGROUND:

Rare disorders comprise of ~ 7500 different conditions affecting multiple systems. Diagnosis of rare diseases is complex due to dearth of specialized medical professionals, testing labs and limited therapeutic options. There is scarcity of data on the prevalence of rare diseases in different populations. India being home to a large population comprising of 4600 population groups, of which several thousand are endogamous, is likely to have a high burden of rare diseases. The present study provides a retrospective overview of a cohort of patients with rare genetic diseases identified at a tertiary genetic test centre in India.

RESULTS:

Overall, 3294 patients with 305 rare diseases were identified in the present study cohort. These were categorized into 14 disease groups based on the major organ/ organ system affected. Highest number of rare diseases (D = 149/305, 48.9%) were identified in the neuromuscular and neurodevelopmental (NMND) group followed by inborn errors of metabolism (IEM) (D = 47/305; 15.4%). Majority patients in the present cohort (N = 1992, 61%) were diagnosed under IEM group, of which Gaucher disease constituted maximum cases (N = 224, 11.2%). Under the NMND group, Duchenne muscular dystrophy (N = 291/885, 32.9%), trinucleotide repeat expansion disorders (N = 242/885; 27.3%) and spinal muscular atrophy (N = 141/885, 15.9%) were the most common. Majority cases of ß-thalassemia (N = 120/149, 80.5%) and cystic fibrosis (N = 74/75, 98.7%) under the haematological and pulmonary groups were observed, respectively. Founder variants were identified for Tay-Sachs disease and mucopolysaccharidosis IVA diseases. Recurrent variants for Gaucher disease (GBAc.1448T > C), ß-thalassemia (HBBc.92.+5G > C), non-syndromic hearing loss (GJB2c.71G > A), albinism (TYRc.832 C > T), congenital adrenal hyperplasia (CYP21A2c.29-13 C > G) and progressive pseudo rheumatoid dysplasia (CCN6c.298T > A) were observed in the present study.

CONCLUSION:

The present retrospective study of rare disease patients diagnosed at a tertiary genetic test centre provides first insight into the distribution of rare genetic diseases across the country. This information will likely aid in drafting future health policies, including newborn screening programs, development of target specific panel for affordable diagnosis of rare diseases and eventually build a platform for devising novel treatment strategies for rare diseases.
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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Doenças Raras Idioma: En Ano de publicação: 2024 Tipo de documento: Article
Texto completo
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XML
PubMed Links
Buscar no Google

Texto completo: 1 Base de dados: MEDLINE Assunto principal: Doenças Raras Idioma: En Ano de publicação: 2024 Tipo de documento: Article