Understanding Human Cerebral Malaria through a Blood Transcriptomic Signature: Evidences for Erythrocyte Alteration, Immune/Inflammatory Dysregulation, and Brain Dysfunction

Cabantous, Stéphanie; Poudiougou, Belco; Bergon, Aurélie; Barry, Abdoulaye; Oumar, Aboubacar Alassane; Traore, A.; Chevillard, Christophe; Doumbo, Ogobara K.; Dessein, Alain; Marquet, Sandrine

doi:10.1155/2020/3280689

Cited by 13 publications

(22 citation statements)

References 49 publications

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“…This means MM and some neurodegenerative diseases may share parallel biological processes, which is contradictory to the findings of Thiam et al . [ 28 ] and Cabantous et al [ 29 ], where neurodegenerative pathways were found in CM only. Nonetheless, processes involved in cancer, EBV infection and DNA damage repair were the most significant.…”

Section: Discussionmentioning

confidence: 99%

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Transcriptome-based analysis of blood samples reveals elevation of DNA damage response, neutrophil degranulation, cancer and neurodegenerative pathways in Plasmodium falciparum patients

Karikari

Wruck

Adjaye

2021

Malar J

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Background Malaria caused by Plasmodium falciparum results in severe complications including cerebral malaria (CM) especially in children. While the majority of falciparum malaria survivors make a full recovery, there are reports of some patients ending up with neurological sequelae or cognitive deficit. Methods An analysis of pooled transcriptome data of whole blood samples derived from two studies involving various P. falciparum infections, comprising mild malaria (MM), non-cerebral severe malaria (NCM) and CM was performed. Pathways and gene ontologies (GOs) elevated in the distinct P. falciparum infections were determined. Results In all, 2876 genes were expressed in common between the 3 forms of falciparum malaria, with CM having the least number of expressed genes. In contrast to other research findings, the analysis from this study showed MM share similar biological processes with cancer and neurodegenerative diseases, NCM is associated with drug resistance and glutathione metabolism and CM is correlated with endocannabinoid signalling and non-alcoholic fatty liver disease (NAFLD). GO revealed the terms biogenesis, DNA damage response and IL-10 production in MM, down-regulation of cytoskeletal organization and amyloid-beta clearance in NCM and aberrant signalling, neutrophil degranulation and gene repression in CM. Differential gene expression analysis between CM and NCM showed the up-regulation of neutrophil activation and response to herbicides, while regulation of axon diameter was down-regulated in CM. Conclusions Results from this study reveal that P. falciparum-mediated inflammatory and cellular stress mechanisms may impair brain function in MM, NCM and CM. However, the neurological deficits predominantly reported in CM cases could be attributed to the down-regulation of various genes involved in cellular function through transcriptional repression, axonal dysfunction, dysregulation of signalling pathways and neurodegeneration. It is anticipated that the data from this study, might form the basis for future hypothesis-driven malaria research.

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Section: Discussionmentioning

confidence: 99%

“…and Cabantous et al . demonstrated the activation of genes associated with AD and PD in CM [ 28 , 29 ]. In addition, Boldt et al .…”

Section: Introductionmentioning

confidence: 99%

Transcriptome-based analysis of blood samples reveals elevation of DNA damage response, neutrophil degranulation, cancer and neurodegenerative pathways in Plasmodium falciparum patients

Karikari

Wruck

Adjaye

2021

Malar J

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“…The protein interaction network besides relevant sub-networks of IL-18 signaling and the blood group proteins XK and KEL regulating axon diameter showed a large connected area centered by TUBB2A and the Metalloproteinases 8 and 9 (MMP8, MMP9). TUBB2A has been reported to be up-regulated in CM by Cabantous et al [29] as part of the Parkin-Ubiquitin proteasome degradation pathway which when impaired can be deleterious to dopaminergic neurons [114].…”

Section: Discussionmentioning

confidence: 97%

“…The copyright holder for this preprint this version posted June 16, 2021. ; https://doi.org/10.1101/2021.06. 16.448682 doi: bioRxiv preprint and Cabantous et al demonstrated the activation of genes associated with AD and PD in CM [28,29]. In addition, Boldt et al found a signature of 22 differentially expressed genes related to immunopathological processes and complement regulation in the transcriptome of distinct conditions of childhood malaria including CM [30].…”

Section: Introductionmentioning

confidence: 99%

Inflammation and Cellular Stress Induced Neurological Sequelae ofPlasmodium falciparumMalaria

Wruck

Adjaye

2021

Preprint

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Background: Malaria caused by Plasmodium falciparum results in severe complications including cerebral malaria (CM) especially in children. While the majority of falciparum malaria survivors make a full recovery, there are reports of some patients ending up with neurological sequelae. Methods: We performed an analysis of pooled transcriptome data of whole blood samples derived from two studies involving various Plasmodium falciparum infections, comprising mild malaria (MM), non-cerebral severe malaria (NCM) and CM. Pathways and gene ontologies (GOs) elevated in the distinct falciparum infections were identified. Results: Contrary to other research findings, our analysis showed MM share similar biological processes with cancer and neurodegenerative diseases, NCM is associated with drug resistance and glutathione metabolism and CM is correlated with endocannabinoid signaling and non-alcoholic fatty liver disease (NAFLD). GO revealed the terms biogenesis, DNA damage response and IL-10 production in MM, down-regulation of cytoskeletal organization and amyloid-beta clearance in NCM and aberrant signaling, neutrophil degranulation and gene repression in CM. Differential gene expression analysis between CM and NCM showed the up-regulation of neutrophil activation and response to herbicides while regulation of axon diameter was down-regulated in CM. Conclusions: The results of this study have demonstrated that the deleterious effect of falciparum malaria on the brain may not be limited to CM and NCM alone but also MM. However, the severity of neurological deficit in CM might be due to the down-regulation of various genes involved in cellular function through transcriptional repression, axonal dysfunction, dysregulation of signaling pathways and neurodegeneration as a result of inflammation and cellular stress. We anticipate that our data might form the basis for future hypothesis-driven malaria research.

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“…As molecular processes driving complex diseases usually involve sets of genes acting in a concerted way, one strategy is to use high-throughput “omics” technologies to simultaneously investigate thousands of genes in a pathological context [ 6 ]. In human medicine, it has been observed that the analysis of the blood transcriptome can provide a comprehensive view of the state of the immune system, advance our understanding of disease pathogenesis and highlight potential biomarkers to be used in diagnosis, prognosis and treatment monitoring [ 5 , 7 , 8 ].…”

Section: Introductionmentioning

confidence: 99%

Blood Transcriptomics of Turbot Scophthalmus maximus: A Tool for Health Monitoring and Disease Studies

Ronza

Álvarez‐Dios

Robledo

et al. 2021

Animals

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Blood transcriptomics is emerging as a relevant tool to monitor the status of the immune system and assist in diagnosis, prognosis, treatment and pathogenesis studies of diseases. In fish pathology, the potential of transcriptome profiling of blood is still poorly explored. Here, RNA sequencing was applied to analyze the blood transcriptional profile of turbot (Scophthalmus maximus), the most important farmed flatfish. The study was conducted in healthy specimens and specimens parasitized by the myxozoan Enteromyxum scophthalmi, which causes one of the most devastating diseases in turbot aquaculture. The blood of healthy turbot showed a transcriptomic profile mainly related to erythrocyte gas transportation function, but also to antigen processing and presentation. In moderately infected turbot, the blood reflected a broad inhibition of the immune response. Particularly, down-regulation of the B cell receptor signaling pathway was shared with heavily parasitized fish, which showed larger transcriptomic changes, including the activation of the inflammatory response. Turbot response to enteromyxosis proved to be delayed, dysregulated and ineffective in stopping the infection. The study evinces that blood transcriptomics can contribute to a better understanding of the teleost immune system and serve as a reliable tool to investigate the physiopathological status of fish.

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Understanding Human Cerebral Malaria through a Blood Transcriptomic Signature: Evidences for Erythrocyte Alteration, Immune/Inflammatory Dysregulation, and Brain Dysfunction

Cited by 13 publications

References 49 publications

Transcriptome-based analysis of blood samples reveals elevation of DNA damage response, neutrophil degranulation, cancer and neurodegenerative pathways in Plasmodium falciparum patients

Transcriptome-based analysis of blood samples reveals elevation of DNA damage response, neutrophil degranulation, cancer and neurodegenerative pathways in Plasmodium falciparum patients

Inflammation and Cellular Stress Induced Neurological Sequelae ofPlasmodium falciparumMalaria

Blood Transcriptomics of Turbot Scophthalmus maximus: A Tool for Health Monitoring and Disease Studies

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