Structural and functional implications of SLC13A3 and SLC9A6 mutations: an in silico approach to understanding intellectual disability

Syeda Iqra Hussain; Nazif Muhammad; Salah Ud Din Shah; Fardous Fardous; Sher Alam Khan; Niamatullah Khan; Adil U Rehman; Mehwish Siddique; Shoukat Ali Wasan; Rooh Niaz; Hafiz Ullah; Niamat Khan; Noor Muhammad; Muhammad Usman Mirza; Naveed Wasif; Saadullah Khan

doi:10.1186/s12883-023-03397-y

Structural and functional implications of SLC13A3 and SLC9A6 mutations: an in silico approach to understanding intellectual disability

BMC Neurol. 2023 Oct 4;23(1):353. doi: 10.1186/s12883-023-03397-y.

Authors

Syeda Iqra Hussain^#¹, Nazif Muhammad^#¹, Salah Ud Din Shah¹, Fardous Fardous², Sher Alam Khan¹, Niamatullah Khan¹, Adil U Rehman¹, Mehwish Siddique³, Shoukat Ali Wasan⁴, Rooh Niaz¹, Hafiz Ullah⁵, Niamat Khan¹, Noor Muhammad¹, Muhammad Usman Mirza⁶, Naveed Wasif^{7

8}, Saadullah Khan⁹

Affiliations

¹ Department of Biotechnology and Genetic Engineering, Kohat University of Science & Technology (KUST), Kohat, Khyber Pakhtunkhwa, Pakistan.
² Department of Medical Lab Technology, Kohat University of Science & Technology (KUST), Kohat, Khyber Pakhtunkhwa, Pakistan.
³ Department of Zoology, Government Post Graduate College for Women, Satellite Town, Gujranwala, Pakistan.
⁴ Department of Botany, Faculty of Natural Sciences, Shah Abdul Latif University, Khairpur, Sindh, Pakistan.
⁵ Gomal Center of Biochemistry and Biotechnology (GCBB), Gomal University D. I. Khan, D. I. Khan, Pakistan.
⁶ Department of Chemistry and Biochemistry, University of Windsor, Windsor, ON, N9B 1C4, Canada.
⁷ Institute of Human Genetics, Ulm University and Ulm University Medical Center, 89081, Ulm, Germany. naveed.wasif@uksh.de.
⁸ Institute of Human Genetics, University Hospital Schleswig-Holstein, Campus Kiel, Kiel, Germany. naveed.wasif@uksh.de.
⁹ Department of Biotechnology and Genetic Engineering, Kohat University of Science & Technology (KUST), Kohat, Khyber Pakhtunkhwa, Pakistan. saad@kust.edu.pk.

^# Contributed equally.

Abstract

Background: Intellectual disability (ID) is a condition that varies widely in both its clinical presentation and its genetic underpinnings. It significantly impacts patients' learning capacities and lowers their IQ below 70. The solute carrier (SLC) family is the most abundant class of transmembrane transporters and is responsible for the translocation of various substances across cell membranes, including nutrients, ions, metabolites, and medicines. The SLC13A3 gene encodes a plasma membrane-localized Na+/dicarboxylate cotransporter 3 (NaDC3) primarily expressed in the kidney, astrocytes, and the choroid plexus. In addition to three Na + ions, it brings four to six carbon dicarboxylates into the cytosol. Recently, it was discovered that patients with acute reversible leukoencephalopathy and a-ketoglutarate accumulation (ARLIAK) carry pathogenic mutations in the SLC13A3 gene, and the X-linked neurodevelopmental condition Christianson Syndrome is caused by mutations in the SLC9A6 gene, which encodes the recycling endosomal alkali cation/proton exchanger NHE6, also called sodium-hydrogen exchanger-6. As a result, there are severe impairments in the patient's mental capacity, physical skills, and adaptive behavior.

Methods and results: Two Pakistani families (A and B) with autosomal recessive and X-linked intellectual disorders were clinically evaluated, and two novel disease-causing variants in the SLC13A3 gene (NM 022829.5) and the SLC9A6 gene (NM 001042537.2) were identified using whole exome sequencing. Family-A segregated a novel homozygous missense variant (c.1478 C > T; p. Pro493Leu) in the exon-11 of the SLC13A3 gene. At the same time, family-B segregated a novel missense variant (c.1342G > A; p.Gly448Arg) in the exon-10 of the SLC9A6 gene. By integrating computational approaches, our findings provided insights into the molecular mechanisms underlying the development of ID in individuals with SLC13A3 and SLC9A6 mutations.

Conclusion: We have utilized in-silico tools in the current study to examine the deleterious effects of the identified variants, which carry the potential to understand the genotype-phenotype relationships in neurodevelopmental disorders.

Keywords: Acute reversible leukoencephalopathy; Christianson Syndrome; Exome sequencing; Intellectual disability; Molecular dynamics simulation; SLC13A3; SLC9A6.

MeSH terms

Epilepsy* / complications
Humans
Intellectual Disability* / genetics
Ions
Microcephaly* / genetics
Mutation
Pedigree

Substances

Ions