Characterization of mtDNA variation in a cohort of South African paediatric patients with mitochondrial disease

Walt, Elizna M. Van der; Smuts, Izelle; Taylor, Robert W.; Elson, Joanna L.; Turnbull, Doug M.; Louw, R.; Westhuizen, Francois H. van der

doi:10.1038/ejhg.2011.262

Cited by 32 publications

(39 citation statements)

References 39 publications

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“…However, the distribution of mitochondrial haplogroups we found was similar to a recently published South African study conducted in 71 children. 29 None of the participants analyzed belonged to the European mitochondrial haplogroups.…”

Section: Discussionmentioning

confidence: 99%

Mitochondrial Genomics and Antiretroviral Therapy-Associated Metabolic Complications in HIV-Infected Black South Africans: A Pilot Study

Sinxadi

Dave

Samuels

et al. 2013

AIDS Research and Human Retroviruses

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Studies suggest that mitochondrial DNA (mtDNA) haplogroups are associated with antiretroviral therapy (ART)-related metabolic complications and distal sensory polyneuropathy (DSP), but there have been few studies in persons of African descent. We explored such associations in South African adults. Clinical and laboratory data and DNA specimens from a cross-sectional study were used. Sequencing and Phylotree determined African mtDNA subhaplogroups. Wilcoxon and regression analyses determined associations between mtDNA subhaplogroups and ART-related complications. The 171 participants represented six major haplogroups: L0 (n=78), L1 (n=3), L2 (n=30), L3 (n=53), L4 (n=1), and L5 (n=6). Analyses were restricted to 161 participants representing L0, L2, and L3: 78% were female; the median age was 36 years. All had been exposed to thymidine analogues, 42% were on lopinavir/ritonavir (lopinavir/r), and 58% were on either efavirenz or nevirapine. Median (IQR) ART duration was 22 (14-36) months. Median fasting triglycerides were 1.60 (1.13-1.75) and 1.04 (0.83-1.45) mmol/liter among L3e1 (n=22) and other subhaplogroups, respectively (p=0.003). Subhaplogroup L3e1 [adjusted OR (aOR) 3.16 (95% CI: 1.11-8.96); p=0.03] and exposure to lopinavir/r [aOR 2.98 (95% CI: 1.02-8.96); p=0.05] were independently associated with hypertriglyceridemia, after adjusting for age, sex, and ART duration. There were no significant associations between mtDNA haplogroups and cholesterol, dysglycemia, hyperlactatemia, or lipoatrophy, or DSP. Subhaplogroup L3e1 and lopinavir/r exposure were independently associated with hypertriglyceridemia in black South Africans on ART. This is the first report to link an African mtDNA variant with hypertriglyceridemia. If replicated, these findings may provide new insights into host factors affecting metabolic complications.

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Section: Discussionmentioning

confidence: 99%

Mitochondrial Genomics and Antiretroviral Therapy-Associated Metabolic Complications in HIV-Infected Black South Africans: A Pilot Study

Sinxadi

Dave

Samuels

et al. 2013

AIDS Research and Human Retroviruses

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“…So far, high-throughput sequencing has been used to study mitochondrial disorders (Calvo et al, 2012; Vasta et al, 2009); (Dames et al, 2013); (van der Walt et al, 2012), mitochondrial DNA mutations due to radiation (Guo et al, 2012a), heteroplasmy inheritance (Payne et al, 2013), cancer (Yang Ai et al, 2013); (Lam et al, 2012) and many other related fields. Next-generation methods targeting the mitochondrial genome result in very high depth mtDNA sequences, but the ability to detect low-level heteroplasmies is still limited by a number of quality control criteria that must be carefully handled.…”

Section: Discussionmentioning

confidence: 99%

High-throughput sequencing in mitochondrial DNA research

Samuels

Clark

et al. 2014

Mitochondrion

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Next-generation sequencing, also known as high-throughput sequencing, has greatly enhanced researchers’ ability to conduct biomedical research on all levels. Mitochondrial research has also benefitted greatly from high-throughput sequencing; sequencing technology now allows for screening of all 16569 base pairs of the mitochondrial genome simultaneously for SNPs and low level heteroplasmy and, in some cases, the estimation of mitochondrial DNA copy number. It is important to realize the full potential of high-throughput sequencing for the advancement of mitochondrial research. To this end, we review how high-throughput sequencing has impacted mitochondrial research in the categories of SNPs, low level heteroplasmy, copy number, and structural variants. We also discuss the different types of mitochondrial DNA sequencing and their pros and cons. Based on previous studies conducted by various groups, we provide strategies for processing mitochondrial DNA sequencing data, including assembly, variant calling, and quality control.

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“…The advent of cheaper and quicker sequencing technologies is likely to make this even more frequent. Indeed, frequent complete mtDNA sequencing will almost certainly extend beyond nations that are currently offering extensive clinical genetics services [Smuts et al, 2010; van der Walt et al, 2012]. When conducted, complete mtDNA sequencing may reveal a known pathogenic variant, but in some cases no previously confirmed pathogenic mutation is identified, though one or more novel (and potentially pathogenic) changes may be observed.…”

Section: Assessment and Reporting Of Mtdna Variation Seen In Patientsmentioning

confidence: 99%

Toward a mtDNA locus-specific mutation database using the LOVD platform

et al. 2012

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ABSTRACT:The Human Variome Project (HVP) is a global effort to collect and curate all human genetic variation affecting health. Mutations of mitochondrial DNA (mtDNA) are an important cause of neurogenetic disease in humans; however, identification of the pathogenic mutations responsible can be problematic. In this article, we provide explanations as to why and suggest how such difficulties might be overcome. We put forward a case in support of a new Locus Specific Mutation Database (LSDB) implemented using the Leiden Open-source Variation Database (LOVD) system that will not only list primary mutations, but also present the evidence supporting their role in disease. Critically, we feel that this new database should have the capacity to store information on the observed phenotypes alongside the genetic varia-

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Characterization of mtDNA variation in a cohort of South African paediatric patients with mitochondrial disease

Cited by 32 publications

References 39 publications

Mitochondrial Genomics and Antiretroviral Therapy-Associated Metabolic Complications in HIV-Infected Black South Africans: A Pilot Study

Mitochondrial Genomics and Antiretroviral Therapy-Associated Metabolic Complications in HIV-Infected Black South Africans: A Pilot Study

High-throughput sequencing in mitochondrial DNA research

Toward a mtDNA locus-specific mutation database using the LOVD platform

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