Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum
The emergence of parasite resistance to antimalarials has been impeding the efforts in malaria elimination. Continuous surveillance of treatment failures from the clinical population informs the efficacy of the currently used antimalarial treatment and provide essential clues in deciphering the m...
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sg-ntu-dr.10356-1563572023-02-28T18:33:04Z Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum Assisi, Christina Zbynek Bozdech School of Biological Sciences ZBozdech@ntu.edu.sg Science::Biological sciences::Genetics Science::Biological sciences::Molecular biology Science::Biological sciences::Microbiology::Drug Resistance The emergence of parasite resistance to antimalarials has been impeding the efforts in malaria elimination. Continuous surveillance of treatment failures from the clinical population informs the efficacy of the currently used antimalarial treatment and provide essential clues in deciphering the molecular mechanism of resistance. Screening of resistance biomarkers from clinical isolates has undermined the identification of large genetic variants, mainly due to technical challenges imposed by low quantity of genetic material and low complexity Plasmodium genome, making the analysis prone to bias. This study screened large genetic structural variations from 413 clinical samples collected in Greater Mekong Subregions, the epicentre of antimalarial treatment failures. Samples were obtained in collaboration with Tracking Resistance to Artemisinin Collaboration (TRAC) studies. Large structural variants were screened using an optimized microarray based Comparative Genomic Hybridization (aCGH) technique. We identified Copy Number Amplification in pfmdr1, pfgch1, and pfpm2, previously reported in association with mainly Mefloquine, Sulfadoxine-Pyrimethamine, and Piperaquine resistance, respectively. In addition, we also identified novel CNV in pfvit and pfyhm2 within the same locus, known for function in iron detoxification and mitochondrial electron transport chain, respectively. Four variant genes: pfpm2, pfvit, pfcyp19b, and pfk13, were chosen for biological and phenotypical characterization using an in vitro parasite model. The overall work suggested the CYP19B as a potential downstream effector of K13 C580Y allele as well as PMII and K13 probable compensatory/synergistic relationship in Ring stage; the stage had been shown to exhibit reduced susceptibility to Artemisinin treatment. Collectively, this work presented an additional potential molecular mechanism to the current notion of antimalarial resistance. Doctor of Philosophy 2022-04-13T06:52:08Z 2022-04-13T06:52:08Z 2021 Thesis-Doctor of Philosophy Assisi, C. (2021). Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum. Doctoral thesis, Nanyang Technological University, Singapore. https://hdl.handle.net/10356/156357 https://hdl.handle.net/10356/156357 10.32657/10356/156357 en This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License (CC BY-NC 4.0). application/pdf Nanyang Technological University |
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Science::Biological sciences::Genetics Science::Biological sciences::Molecular biology Science::Biological sciences::Microbiology::Drug Resistance Assisi, Christina Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum |
| description |
The emergence of parasite resistance to antimalarials has been impeding the
efforts in malaria elimination. Continuous surveillance of treatment failures from
the clinical population informs the efficacy of the currently used antimalarial
treatment and provide essential clues in deciphering the molecular mechanism
of resistance. Screening of resistance biomarkers from clinical isolates has
undermined the identification of large genetic variants, mainly due to technical
challenges imposed by low quantity of genetic material and low complexity
Plasmodium genome, making the analysis prone to bias.
This study screened large genetic structural variations from 413 clinical samples
collected in Greater Mekong Subregions, the epicentre of antimalarial treatment
failures. Samples were obtained in collaboration with Tracking Resistance to
Artemisinin Collaboration (TRAC) studies. Large structural variants were screened
using an optimized microarray based Comparative Genomic Hybridization
(aCGH) technique. We identified Copy Number Amplification in pfmdr1, pfgch1,
and pfpm2, previously reported in association with mainly Mefloquine,
Sulfadoxine-Pyrimethamine, and Piperaquine resistance, respectively. In addition,
we also identified novel CNV in pfvit and pfyhm2 within the same locus, known
for function in iron detoxification and mitochondrial electron transport chain,
respectively.
Four variant genes: pfpm2, pfvit, pfcyp19b, and pfk13, were chosen for biological
and phenotypical characterization using an in vitro parasite model. The overall
work suggested the CYP19B as a potential downstream effector of K13 C580Y
allele as well as PMII and K13 probable compensatory/synergistic relationship in
Ring stage; the stage had been shown to exhibit reduced susceptibility to
Artemisinin treatment. Collectively, this work presented an additional potential
molecular mechanism to the current notion of antimalarial resistance. |
| author2 |
Zbynek Bozdech |
| author_facet |
Zbynek Bozdech Assisi, Christina |
| format |
Thesis-Doctor of Philosophy |
| author |
Assisi, Christina |
| author_sort |
Assisi, Christina |
| title |
Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum |
| title_short |
Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum |
| title_full |
Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum |
| title_fullStr |
Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum |
| title_full_unstemmed |
Screening and characterization of antimalarial resistance related genetic structural variations in P. falciparum |
| title_sort |
screening and characterization of antimalarial resistance related genetic structural variations in p. falciparum |
| publisher |
Nanyang Technological University |
| publishDate |
2022 |
| url |
https://hdl.handle.net/10356/156357 |
| _version_ |
1759853521310580736 |