Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria

Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria

Background: A tremendous level of success has been achieved since the introduction of chloroquine and the combination of amodiaquine and artemisinin for the treatment of both complicated and uncomplicated malaria infections in sub-Saharan Africa. However, the recent discovery of drug resistant strai...

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Main Authors: Olalere Shittu, Olufunke Adenike Opeyemi, Olumuyiwa Babagbemi Omotesho, Oluwatosin Fakayode, Nnaemeka Asogwa, Opeyemi Margaret Adeniyi, Ifeoluwa Margaret Fatoba, Kayode Muritala Salawu, Olusola Ajibaye, Olarewaju Abdulkareem Babamale, Oluyinka Ajibola Iyiola, Olusola Isaac Aremu
Format: Article
Language:English
Published: Karolinum Press 2020-01-01
Series:Acta Medica
Subjects:
Plasmodium falciparum
Chloroquine
Amodiaquine-Artemisinin combination therapy
CYP2C8*2
Hausa
Igbo
Online Access:https://actamedica.lfhk.cuni.cz/63/3/0119/
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spelling doaj-82827896d00c442dba9019dc5cafd85a2020-11-25T03:53:46ZengKarolinum PressActa Medica1211-42861805-96942020-01-0163311912310.14712/18059694.2020.29Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, NigeriaOlalere Shittu0Olufunke Adenike Opeyemi1Olumuyiwa Babagbemi Omotesho2Oluwatosin Fakayode3Nnaemeka Asogwa4Opeyemi Margaret Adeniyi5Ifeoluwa Margaret Fatoba6Kayode Muritala Salawu7Olusola Ajibaye8Olarewaju Abdulkareem Babamale9Oluyinka Ajibola Iyiola10Olusola Isaac Aremu11Parasitology Unit, Department of Zoology, University of Ilorin, Ilorin, NigeriaParasitology Unit, Department of Zoology, University of Ilorin, Ilorin, NigeriaUnilorin Clinic, University of Ilorin, Ilorin, NigeriaChildren Specialist Hospital, Centre Igboro, Ilorin, NigeriaDepartment of Biochemistry, University of Ilorin, Ilorin, NigeriaParasitology Unit, Department of Zoology, University of Ilorin, Ilorin, NigeriaParasitology Unit, Department of Zoology, University of Ilorin, Ilorin, NigeriaDepartment of Pharmacognosy and Drug Development, University of Ilorin, Ilorin, NigeriaBiochemistry Division, Nigerian Institute of Medical Research, Lagos, NigeriaParasitology Unit, Department of Zoology, University of Ilorin, Ilorin, NigeriaCell Biology and Genetics Unit, Department of Zoology, University of Ilorin, Ilorin, NigeriaDepartment of Pharmaceutics and Industrial Pharmacy, Faculty of Pharmaceutical Sciences, University of Ilorin, Ilorin, NigeriaBackground: A tremendous level of success has been achieved since the introduction of chloroquine and the combination of amodiaquine and artemisinin for the treatment of both complicated and uncomplicated malaria infections in sub-Saharan Africa. However, the recent discovery of drug resistant strains of Plasmodium falciparum (P.f.) and the ability of the parasite to ingest CYP2C8 into its digestive vacuole is of great public health concern. This study probes the occurrence of CYP2C8*2 allelic mutant amongst malaria patients in North-Central Nigeria. Methods: Three hundred and eighty five (385) unrelated study participants were screened for current malaria episodes using routine microscopy and/or rapid diagnostic test strips (RDTs). Chelex extraction method was used for single nucleotide polymorphisms (SNPs) and identification of CYP2C8*2 (805A > T) variant respectively. Wild-type (A) and the defective allele (T) were differentiated with the use of Polymerase Chain Reaction-Restriction Fragment Length Polymorphism (PCR-RFLP). The results obtained were further validated with Sanger sequencing of a few samples and thereafter, the genotype data were statistically processed. All alleles obtained were in Hardy Weinberg equilibrium. Results: Out of the 385 participants (45.5% Male and 54.5% Female) genotyped for SNPs, 75 (19.5%) had the autosomal recessive mutant trait. Occurrence of mutant traits was gender and ethnic independent (p > 0.05). Yoruba ethnic group recorded a reduction in proportion of genotypic defective CYP2C8*2 allele (T) (1 in every 8 persons) with a carrier percentage of 13.3% compared with Hausa (26.62%); Igbo (25.37%) and other minority ethnic groups (17.6%). Conclusions: A remarkable inter-ethnic differences in autosomal recessive CYP2C8*2 allele was observed. By implication, there is a gradual incursion of genetic drift for poor CQ and AQ-Artemisinin metabolizers among the inhabitants.https://actamedica.lfhk.cuni.cz/63/3/0119/Plasmodium falciparumChloroquineAmodiaquine-Artemisinin combination therapyCYP2C8*2HausaIgbo
collection DOAJ
language English
format Article
sources DOAJ
author Olalere Shittu
Olufunke Adenike Opeyemi
Olumuyiwa Babagbemi Omotesho
Oluwatosin Fakayode
Nnaemeka Asogwa
Opeyemi Margaret Adeniyi
Ifeoluwa Margaret Fatoba
Kayode Muritala Salawu
Olusola Ajibaye
Olarewaju Abdulkareem Babamale
Oluyinka Ajibola Iyiola
Olusola Isaac Aremu
spellingShingle Olalere Shittu
Olufunke Adenike Opeyemi
Olumuyiwa Babagbemi Omotesho
Oluwatosin Fakayode
Nnaemeka Asogwa
Opeyemi Margaret Adeniyi
Ifeoluwa Margaret Fatoba
Kayode Muritala Salawu
Olusola Ajibaye
Olarewaju Abdulkareem Babamale
Oluyinka Ajibola Iyiola
Olusola Isaac Aremu
Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria
Acta Medica
Plasmodium falciparum
Chloroquine
Amodiaquine-Artemisinin combination therapy
CYP2C8*2
Hausa
Igbo
author_facet Olalere Shittu
Olufunke Adenike Opeyemi
Olumuyiwa Babagbemi Omotesho
Oluwatosin Fakayode
Nnaemeka Asogwa
Opeyemi Margaret Adeniyi
Ifeoluwa Margaret Fatoba
Kayode Muritala Salawu
Olusola Ajibaye
Olarewaju Abdulkareem Babamale
Oluyinka Ajibola Iyiola
Olusola Isaac Aremu
author_sort Olalere Shittu
title Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria
title_short Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria
title_full Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria
title_fullStr Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria
title_full_unstemmed Clinical Probe of Cyp2C8*2 Mutants in a Malaria Hyperendemic Zone: Evidence from North-Central, Nigeria
title_sort clinical probe of cyp2c8*2 mutants in a malaria hyperendemic zone: evidence from north-central, nigeria
publisher Karolinum Press
series Acta Medica
issn 1211-4286
1805-9694
publishDate 2020-01-01
description Background: A tremendous level of success has been achieved since the introduction of chloroquine and the combination of amodiaquine and artemisinin for the treatment of both complicated and uncomplicated malaria infections in sub-Saharan Africa. However, the recent discovery of drug resistant strains of Plasmodium falciparum (P.f.) and the ability of the parasite to ingest CYP2C8 into its digestive vacuole is of great public health concern. This study probes the occurrence of CYP2C8*2 allelic mutant amongst malaria patients in North-Central Nigeria. Methods: Three hundred and eighty five (385) unrelated study participants were screened for current malaria episodes using routine microscopy and/or rapid diagnostic test strips (RDTs). Chelex extraction method was used for single nucleotide polymorphisms (SNPs) and identification of CYP2C8*2 (805A > T) variant respectively. Wild-type (A) and the defective allele (T) were differentiated with the use of Polymerase Chain Reaction-Restriction Fragment Length Polymorphism (PCR-RFLP). The results obtained were further validated with Sanger sequencing of a few samples and thereafter, the genotype data were statistically processed. All alleles obtained were in Hardy Weinberg equilibrium. Results: Out of the 385 participants (45.5% Male and 54.5% Female) genotyped for SNPs, 75 (19.5%) had the autosomal recessive mutant trait. Occurrence of mutant traits was gender and ethnic independent (p > 0.05). Yoruba ethnic group recorded a reduction in proportion of genotypic defective CYP2C8*2 allele (T) (1 in every 8 persons) with a carrier percentage of 13.3% compared with Hausa (26.62%); Igbo (25.37%) and other minority ethnic groups (17.6%). Conclusions: A remarkable inter-ethnic differences in autosomal recessive CYP2C8*2 allele was observed. By implication, there is a gradual incursion of genetic drift for poor CQ and AQ-Artemisinin metabolizers among the inhabitants.
topic Plasmodium falciparum
Chloroquine
Amodiaquine-Artemisinin combination therapy
CYP2C8*2
Hausa
Igbo
url https://actamedica.lfhk.cuni.cz/63/3/0119/
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