Neuronal Ceroid Lipofuscinosis: Clinical and Laboratory Profile in Children from Tertiary Care Centre in South India

Gowda, Vykuntaraju K; Vegda, Hemadri; Sugumar, Kiruthiga; Gayathri, Narayanappa; Srinivasan, Varunvenkat M.; Santhoshkumar, Rashmi; Bhat, Maya; Balu, S; Naveen, Mohan Rao

doi:10.1055/s-0040-1715575

Cited by 12 publications

(9 citation statements)

References 27 publications

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“…Thus, a multimode approach played a role in the diagnosis of NCL." 1 We agree that observations in the present report might be clinically useful. Some clinical features might be more common in CLN1, whereas others are more common in CLN2.…”

supporting

confidence: 92%

“…We would like to share ideas on “Neuronal Ceroid Lipofuscinosis: Clinical and Laboratory Profile in Children from Tertiary Care Centre in South India.” 1 Prajapati et al noted that “Infantile onset with thalamic atrophy on MRI is common in CLN1 and refractory epilepsy, visual impairment, and specific EEG changes are common … diagnosis and genetic testing in subtyping. Thus, a multimode approach played a role in the diagnosis of NCL.” 1 We agree that observations in the present report might be clinically useful. Some clinical features might be more common in CLN1, whereas others are more common in CLN2.…”

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confidence: 99%

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Ceroid Lipofuscinosis in Children: Correspondence

Sookaromdee¹,

Wiwanitkit

2022

J Pediatr Genet

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confidence: 92%

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confidence: 99%

Ceroid Lipofuscinosis in Children: Correspondence

Sookaromdee¹,

Wiwanitkit

2022

J Pediatr Genet

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“…Pathogenic mutations in CLN genes ( CLN1 , CLN2 , CLN3 , CLN5 , CLN6 , CLN7 , CLN8 , CLN10 , CLN13 , CLN14 , and CLCN2 ) represent the principle contribution among the investigated mutations, and affected patients were of age ranged from 2 to 11 years old. The main clinical features assigned to them were developmental regression, epilepsy, speech impairment, cognitive decline, vision loss, hypotonia, myoclonus, seizures, and ataxia, and their MRI scan showed cerebellar-cerebral atrophy [ 21 ]. Five novel homozygous missense mutations were reported in different genes of 5 unrelated patients; one of them c.600 G > A (p.Trp200Ser) was detected in CLN7 gene using the Sanger sequencing technique only, and the other 4 mutations c.872A > G (p.Gln 291 Arg), c.886G > C (p.Asp296His), c.446G > A (p.Gly149Asp), and (c.906 + 2 T > A) were described in genes CLN1 , CLN7 , CLN14 , and donor splice region of intron 11 of CLN3 gene, respectively, using WES.…”

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confidence: 99%

Whole exome screening of neurodevelopmental regression disorders in a cohort of Egyptian patients

et al. 2022

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Developmental regression describes a child who begins to lose his previously acquired milestones skills after he has reached a certain developmental stage and though affects his childhood development. It is associated with neurodegenerative diseases including leukodystrophy and neuronal ceroid lipofuscinosis diseases (NCLs), one of the most frequent childhood-onset neurodegenerative disorders. The current study focused on screening causative genes of developmental regression diseases comprising neurodegenerative disorders in Egyptian patients using next-generation sequencing (NGS)-based analyses as well as developing checklist to support clinicians who are not familiar with these diseases. A total of 763 Egyptian children (1 to 11 years), mainly diagnosed with developmental regression, seizures, or visual impairment, were studied using whole exome sequencing (WES). Among 763 Egyptian children, 726 cases were early clinically and molecularly diagnosed, including 482 cases that had pediatric stroke, congenital infection, and hepatic encephalopathy; meanwhile, 192 had clearly dysmorphic features, 31 showed central nervous system (CNS) malformation, 17 were diagnosed by leukodystrophy, 2 had ataxia telangiectasia, and 2 were diagnosed with tuberous sclerosis. The remained 37 out of 763 candidates were suspected with NCLs symptoms; however, 28 were confirmed to be NCLs patients, 1 was Kaya-Barakat-Masson syndrome, 1 was diagnosed as infantile neuroaxonal dystrophy, and 7 cases required further molecular diagnosis. This study provided an NGS-based approach of the genetic causes of developmental regression and neurodegenerative diseases as it comprised different variants and de novo mutations with complex phenotypes of these diseases which in turn help in early diagnoses and counseling for affected families.

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confidence: 99%

“…We thank readers for critically evaluating our research study. 1 The queries raised are addressed below.…”

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Ceroid Lipofuscinosis in Children: Author's Reply

Gowda

2022

J Pediatr Genet

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We thank readers for critically evaluating our research study. 1 The queries raised are addressed below.We agree with reviewers' comments on clinical features that might not be able to discriminate and might not be helpful in selecting enzyme assay for CLN1 versus CLN2. Kamate et al reported that thalamic hypointensity is common in CLN1 similar to our cohort. 2 Along with clinical features, neuroimaging features and electroencephalograph findings are helpful in selecting enzyme assay in developing countries where financial constraint is a major factor for genetic testing.

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Neuronal Ceroid Lipofuscinosis: Clinical and Laboratory Profile in Children from Tertiary Care Centre in South India

Cited by 12 publications

References 27 publications

Ceroid Lipofuscinosis in Children: Correspondence

Ceroid Lipofuscinosis in Children: Correspondence

Whole exome screening of neurodevelopmental regression disorders in a cohort of Egyptian patients

Ceroid Lipofuscinosis in Children: Author's Reply

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