Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects

Mitochondrial disorders (MIDs) shows overlapping clinical presentations owing to the genetic and metabolic defects of mitochondria. However, specific relationship between inherited mutations in nuclear encoded mitochondrial proteins and their functional impacts in terms of metabolic defects in patie...

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Autores principales: Gaboon, Nagwa E.A., Banaganapalli, Babajan, Nasser, Khalidah, Razeeth, Mohammed, Alsaedi, Mosab S., Rashidi, Omran M., Abdelwehab, Lereen S., Alahmadi, Turki Saad, Safdar, Osama Y., Shaik, Jilani, Choudhry, Hani M.Z., Al-numan, Huda Husain, Khan, Mohammad Imran, Al-Aama, Jumana Y., Elango, Ramu, Shaik, Noor A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6933272/
https://www.ncbi.nlm.nih.gov/pubmed/31889854
http://dx.doi.org/10.1016/j.sjbs.2019.10.001
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author Gaboon, Nagwa E.A.
Banaganapalli, Babajan
Nasser, Khalidah
Razeeth, Mohammed
Alsaedi, Mosab S.
Rashidi, Omran M.
Abdelwehab, Lereen S.
Alahmadi, Turki Saad
Safdar, Osama Y.
Shaik, Jilani
Choudhry, Hani M.Z.
Al-numan, Huda Husain
Khan, Mohammad Imran
Al-Aama, Jumana Y.
Elango, Ramu
Shaik, Noor A.
author_facet Gaboon, Nagwa E.A.
Banaganapalli, Babajan
Nasser, Khalidah
Razeeth, Mohammed
Alsaedi, Mosab S.
Rashidi, Omran M.
Abdelwehab, Lereen S.
Alahmadi, Turki Saad
Safdar, Osama Y.
Shaik, Jilani
Choudhry, Hani M.Z.
Al-numan, Huda Husain
Khan, Mohammad Imran
Al-Aama, Jumana Y.
Elango, Ramu
Shaik, Noor A.
author_sort Gaboon, Nagwa E.A.
collection PubMed
description Mitochondrial disorders (MIDs) shows overlapping clinical presentations owing to the genetic and metabolic defects of mitochondria. However, specific relationship between inherited mutations in nuclear encoded mitochondrial proteins and their functional impacts in terms of metabolic defects in patients is not yet well explored. Therefore, using high throughput whole exome sequencing (WES), we screened a chronic kidney disease (CKD) and sensorineural hearing loss (SNHL) patient, and her family members to ascertain the mode of inheritance of the mutation, and healthy population controls to establish its rare frequency. The impact of mutation on biophysical characteristics of the protein was further studied by mapping it in 3D structure. Furthermore, LC-MS tandem mass spectrophotometry based untargeted metabolomic profiling was done to study the fluctuations in plasma metabolites relevant to disease causative mutations and kidney damage. We identified a very rare homozygous c.631G > A (p.Val211Met) pathogenic mutation in RMND1 gene in the proband, which is inherited in an autosomal recessive fashion. This gene is involved in the mitochondrial translational pathways and contribute in mitochondrial energy metabolism. The p.Val211Met mutation is found to disturb the structural orientation (RMSD is −2.95 Å) and stability (ΔΔG is −0.552 Kcal/mol) of the RMND1 protein. Plasma metabolomics analysis revealed the aberrant accumulation of metabolites connected to lipid and amino acid metabolism pathways. Of these metabolites, pathway networking has discovered ceramide, a metabolite of sphingolipids, which plays a role in different signaling cascades including mitochondrial membrane biosynthesis, is highly elevated in this patient. This study suggests that genetic defects in RMND1 gene alters the mitochondrial energy metabolism leading to the accumulation of ceramide, and subsequently promote dysregulated apoptosis and tissue necrosis in kidneys.
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spelling pubmed-69332722019-12-30 Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects Gaboon, Nagwa E.A. Banaganapalli, Babajan Nasser, Khalidah Razeeth, Mohammed Alsaedi, Mosab S. Rashidi, Omran M. Abdelwehab, Lereen S. Alahmadi, Turki Saad Safdar, Osama Y. Shaik, Jilani Choudhry, Hani M.Z. Al-numan, Huda Husain Khan, Mohammad Imran Al-Aama, Jumana Y. Elango, Ramu Shaik, Noor A. Saudi J Biol Sci Article Mitochondrial disorders (MIDs) shows overlapping clinical presentations owing to the genetic and metabolic defects of mitochondria. However, specific relationship between inherited mutations in nuclear encoded mitochondrial proteins and their functional impacts in terms of metabolic defects in patients is not yet well explored. Therefore, using high throughput whole exome sequencing (WES), we screened a chronic kidney disease (CKD) and sensorineural hearing loss (SNHL) patient, and her family members to ascertain the mode of inheritance of the mutation, and healthy population controls to establish its rare frequency. The impact of mutation on biophysical characteristics of the protein was further studied by mapping it in 3D structure. Furthermore, LC-MS tandem mass spectrophotometry based untargeted metabolomic profiling was done to study the fluctuations in plasma metabolites relevant to disease causative mutations and kidney damage. We identified a very rare homozygous c.631G > A (p.Val211Met) pathogenic mutation in RMND1 gene in the proband, which is inherited in an autosomal recessive fashion. This gene is involved in the mitochondrial translational pathways and contribute in mitochondrial energy metabolism. The p.Val211Met mutation is found to disturb the structural orientation (RMSD is −2.95 Å) and stability (ΔΔG is −0.552 Kcal/mol) of the RMND1 protein. Plasma metabolomics analysis revealed the aberrant accumulation of metabolites connected to lipid and amino acid metabolism pathways. Of these metabolites, pathway networking has discovered ceramide, a metabolite of sphingolipids, which plays a role in different signaling cascades including mitochondrial membrane biosynthesis, is highly elevated in this patient. This study suggests that genetic defects in RMND1 gene alters the mitochondrial energy metabolism leading to the accumulation of ceramide, and subsequently promote dysregulated apoptosis and tissue necrosis in kidneys. Elsevier 2020-01 2019-10-18 /pmc/articles/PMC6933272/ /pubmed/31889854 http://dx.doi.org/10.1016/j.sjbs.2019.10.001 Text en © 2019 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Gaboon, Nagwa E.A.
Banaganapalli, Babajan
Nasser, Khalidah
Razeeth, Mohammed
Alsaedi, Mosab S.
Rashidi, Omran M.
Abdelwehab, Lereen S.
Alahmadi, Turki Saad
Safdar, Osama Y.
Shaik, Jilani
Choudhry, Hani M.Z.
Al-numan, Huda Husain
Khan, Mohammad Imran
Al-Aama, Jumana Y.
Elango, Ramu
Shaik, Noor A.
Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects
title Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects
title_full Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects
title_fullStr Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects
title_full_unstemmed Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects
title_short Exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed RMND1 mutation induced sphingolipid metabolism defects
title_sort exome sequencing and metabolomic analysis of a chronic kidney disease and hearing loss patient family revealed rmnd1 mutation induced sphingolipid metabolism defects
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6933272/
https://www.ncbi.nlm.nih.gov/pubmed/31889854
http://dx.doi.org/10.1016/j.sjbs.2019.10.001
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