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Open AccessJournal ArticleDOI

Expression Patterns of Plasmodium falciparum Clonally Variant Genes at the Onset of a Blood Infection in Malaria-Naive Humans.

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TLDR
In this paper, the authors provided a detailed characterization of the complete P. falciparum transcriptome across the full intraerythrocytic development cycle (IDC) at the onset of a blood infection in malaria-naive human volunteers.
Abstract
Clonally variant genes (CVGs) play fundamental roles in the adaptation of Plasmodium falciparum to fluctuating conditions of the human host. However, their expression patterns under the natural conditions of the blood circulation have been characterized in detail for only a few specific gene families. Here, we provide a detailed characterization of the complete P. falciparum transcriptome across the full intraerythrocytic development cycle (IDC) at the onset of a blood infection in malaria-naive human volunteers. We found that the vast majority of transcriptional differences between parasites obtained from the volunteers and the parental parasite line maintained in culture occurred in CVGs. In particular, we observed a major increase in the transcript levels of most genes of the pfmc-2tm and gbp families and of specific genes of other families, such as phist, hyp10, rif, or stevor, in addition to previously reported changes in var and clag3 gene expression. Increased transcript levels of individual pfmc-2tm, rif, and stevor genes involved activation in small subsets of parasites. Large transcriptional differences correlated with changes in the distribution of heterochromatin, confirming their epigenetic nature. Furthermore, the similar expression of several CVGs between parasites collected at different time points along the blood infection suggests that the epigenetic memory for multiple CVG families is lost during transmission stages, resulting in a reset of their transcriptional state. Finally, the CVG expression patterns observed in a volunteer likely infected by a single sporozoite suggest that new epigenetic patterns are established during liver stages. IMPORTANCE The ability of malaria parasites to adapt to changes in the human blood environment, where they produce long-term infection associated with clinical symptoms, is fundamental for their survival. CVGs, regulated at the epigenetic level, play a major role in this adaptive process, as changes in the expression of these genes result in alterations in the antigenic and functional properties of the parasites. However, how these genes are expressed under the natural conditions of the human circulation and how their expression is affected by passage through transmission stages are not well understood. Here, we provide a comprehensive characterization of the expression patterns of these genes at the onset of human blood infections, which reveals major differences with in vitro-cultured parasites. We also show that, during transmission stages, the previous expression patterns for many CVG families are lost, and new patterns are established.

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Journal ArticleDOI

Malaria parasites do respond to heat.

TL;DR: The capacity of malaria parasites to respond to changes in their environment at the transcriptional level has been the subject of debate, but recent evidence has unambiguously demonstrated that Plasmodium spp. can produce adaptive transcriptional responses when exposed to some specific types of stress as discussed by the authors .
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Systems biology of malaria explored with nonhuman primates

Mary R. Galinski
- 07 Jun 2022 - 
TL;DR: A review of NHP-NHP infection model systems can be found in this article , with emphasis on modern systems biological approaches to studying longitudinal infections, pathogenesis, immunity, and vaccines.
Journal ArticleDOI

Systems biology of malaria explored with nonhuman primates

Mary R. Galinski
- 07 Jun 2022 - 
TL;DR: A review of NHP-NHP infection model systems can be found in this article , with emphasis on modern systems biological approaches to studying longitudinal infections, pathogenesis, immunity, and vaccines.
Journal ArticleDOI

Selective expression of variant surface antigens enables Plasmodium falciparum to evade immune clearance in vivo

TL;DR: In this paper , the authors used a humanized mouse model to identify parasite factors important for in vivo growth and showed that upregulation of the specific PfEMP1, VAR2CSA, provided the parasite with protection from macrophage phagocytosis and clearance in the humanized mice.
Journal ArticleDOI

CD36—A Host Receptor Necessary for Malaria Parasites to Establish and Maintain Infection

TL;DR: In this paper , the authors discuss why the interaction between PfIEs and CD36 is optimal to maintain a finely regulated equilibrium that allows the parasite to multiply and spread while causing minimal harm to the host in most infections.
References
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Book ChapterDOI

TM4 microarray software suite

TL;DR: This chapter describes each component of the TM4 suite of open‐source tools for data management and reporting, image analysis, normalization and pipeline control, and data mining and visualization and includes a sample analysis walk‐through.
Journal ArticleDOI

The Transcriptome of the Intraerythrocytic Developmental Cycle of Plasmodium falciparum

TL;DR: Analysis of the complete asexual intraerythrocytic developmental cycle (IDC) transcriptome of the HB3 strain of P. falciparum demonstrates that this parasite has evolved an extremely specialized mode of transcriptional regulation that produces a continuous cascade of gene expression, beginning with genes corresponding to general cellular processes, such as protein synthesis, and ending with Plasmodium-specific functionalities.
Journal ArticleDOI

Discovery of Gene Function by Expression Profiling of the Malaria Parasite Life Cycle

TL;DR: A high-density oligonucleotide array is used to generate expression profiles of human and mosquito stages of the malaria parasite's life cycle and finds genes with highly correlated levels and temporal patterns of expression were often involved in similar functions or cellular processes.
Journal ArticleDOI

Bistability, epigenetics, and bet-hedging in bacteria.

TL;DR: Heterogeneous populations can demonstrate increased fitness compared with homogeneous populations and the possible roles of interlinked bistable networks, epigenetic inheritance, and bet-hedging in bacteria are discussed.
Journal ArticleDOI

Antigenic variation in malaria: in situ switching, relaxed and mutually exclusive transcription of var genes during intra‐erythrocytic development in Plasmodium falciparum

TL;DR: The results suggest that an epigenetic mechanism(s) is involved in var gene regulation, and are likely mediated at the level of transcriptional initiation, as demonstrated by nuclear run‐on analyses.
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