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H3K36 methylation reprograms gene expression to drive early gametocyte development in Plasmodium falciparum

Epigenetics Chromatin. 2021-04; 
Jessica Connacher, Gabrielle A Josling, Lindsey M Orchard, Janette Reader, Manuel Llinás, Lyn-Marié Birkholtz
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Catalog Peptides The specificity of commercially obtained ChIP-grade rabbit anti-H3K36me2 (Abcam, ab9049) and anti-H3K36me3 (Abcam, ab9050) antibodies (same batch numbers as previously validated for specificity against H3K36me2&3, [22, 34, 39–41, 43]) was tested using modified and unmodified synthetic peptides (Genscript) of the P. falciparum 3D7 histone H3 sequence as per ENCODE standards Get A Quote

摘要

background: The Plasmodium sexual gametocyte stages are the only transmissible form of the malaria parasite and are thus responsible for the continued transmission of the disease. Gametocytes undergo extensive functional and morphological changes from commitment to maturity, directed by an equally extensive control program. However, the processes that drive the differentiation and development of the gametocyte post-commitment, remain largely unexplored. A previous study reported enrichment of H3K36 di- and tri-methylated (H3K36me2&3) histones in early-stage gametocytes. Using chromatin immunoprecipitation followed by high-throughput sequencing, we identify a stage-specific association between these repressive h... More

关键词

Epigenetics, Gametocyte, H3K36me2, H3K36me3, Histone, Histone demethylation, Histone post-translational modifications, Malaria, Plasmodium