Transcriptomic analysis of human blood samples to identify severity-associated markers in Plasmodium knowlesi malaria
Malaria caused by Plasmodium knowlesi can result in non-severe or severe disease in patients. Transcriptomic-based approaches may provide deeper insights into parasite biology and host immune pathways involved in malaria severity. In our study, the blood transcriptome of P. knowlesi-infecting pat...
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| 格式: | Final Year Project |
| 語言: | English |
| 出版: |
Nanyang Technological University
2022
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| 主題: | |
| 在線閱讀: | https://hdl.handle.net/10356/157268 |
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| 機構: | Nanyang Technological University |
| 語言: | English |
| 總結: | Malaria caused by Plasmodium knowlesi can result in non-severe or severe disease
in patients. Transcriptomic-based approaches may provide deeper insights into
parasite biology and host immune pathways involved in malaria severity. In our
study, the blood transcriptome of P. knowlesi-infecting patients was assessed by
high-throughput sequencing (RNA-seq). The expression profiles associated with
clinical status were analyzed to determine the human differentially expressed genes
(DEGs) and relevant pathways while the changes in leukocyte abundance were
investigated using cell deconvolution. Additionally, a bioinformatics pipeline was
developed to identify malaria-associated viruses and their potential impact on the
severity status of this disease.
We identified 362 human DEGs, which involve various mechanisms including
RNA/protein metabolism and immune cell signaling. Among the identified DEGs,
ALOX5 was successfully validated. Furthermore, decreased proportion of NK cells
and CD8 T cells in severe samples were observed, which contributed to
lymphopenia. Finally, the putative existence of six viruses was found with varying
viral loads, and one of them was correlated with malaria severity. This is the first
study focused on blood transcriptome and the existence of viruses in patients with P.
knowlesi infection; hence, our findings may form a good basis for future research on
this type of malaria. |
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