AI Article Synopsis

  • RbAp46/RBBP7 and RbAp48/RBBP4 are histone chaperones crucial for maintaining chromatin structure, with RbAp48 being a key component of the chromatin assembly factor-1 (CAF-1) complex.
  • A detailed analysis of RbAp46/48 homologs in the malaria parasite Plasmodium falciparum revealed conserved features in their protein structures, indicating evolutionary similarities and differences between species.
  • The study involved cloning and purifying a specific RbAp46/48 protein from P. falciparum, showing its expression in asexual blood stages and its direct interaction with histone H4, enhancing our understanding of these proteins in the biology of the parasite.

Article Abstract

RbAp46/RBBP7 and RbAp48/RBBP4 are WD40-repeat histone chaperones and chromatin adaptors that reside in multiple complexes involved in maintenance of chromatin structure. RbAp48 is the essential subunit of the chromatin assembly factor-1 (CAF-1) complex, therefore also named as CAF-1C. A detailed in silico sequence and structure analysis of homologs of RbAp46/48 in Plasmodium falciparum (PF3D7_0110700 and PF3D7_1433300) exhibited conservation of characteristic features in both the protein-seven-bladed WD40 β-propeller conformation and different binding interfaces. A comparative structural analysis highlighted species-specific features of the parasite, yeast, drosophila, and human RbAp46/48. In the present study, we report cloning, expression, and characterization of P. falciparum PF3D7_0110700, a putative RbAp46/48 (PfRbAp46/48). PfRbAp46/48 was cloned into pTEM11 vector in fusion with 6xHistidine tag and over-expressed in Escherichia coli B834 cells. The protein was purified by Ni-NTA followed by gel permeation chromatography. The protein expressed in all the three asexual blood stages and exhibited nuclear localization. We showed direct interaction of the purified rPfRbAp46/48 with the histone H4. These findings further our understanding of RbAp46/48 proteins and role of these proteins in the parasite biology.

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Source
http://dx.doi.org/10.1007/s00436-020-06669-5DOI Listing

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