Purification of functional Plasmodium falciparum tubulin allows for the identification of parasite-specific microtubule inhibitors

被引:22
作者
Hirst, William G. [1 ,2 ]
Fachet, Dominik [1 ,2 ]
Kuropka, Benno [3 ]
Weise, Christoph [3 ]
Saliba, Kevin J. [2 ]
Reber, Simone [1 ,4 ]
机构
[1] Humboldt Univ, IRI Life Sci, D-10115 Berlin, Germany
[2] Australian Natl Univ, Res Sch Biol, Canberra, ACT 2601, Australia
[3] Free Univ Berlin, Inst Chem & Biochem, Core Facil BioSupraMol, D-14195 Berlin, Germany
[4] Univ Appl Sci Berlin, D-13353 Berlin, Germany
关键词
HUMAN MALARIA PARASITE; SEQUENCE-ANALYSIS; PROTEINS; DINITROANILINE; TYROSINATION; EXPRESSION; INITIATION; HERBICIDES; PLATFORM; DRIVEN;
D O I
10.1016/j.cub.2021.12.049
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Cytoskeletal proteins are essential for parasite proliferation, growth, and transmission, and therefore have the potential to serve as drug targets.(1-5) While microtubules and their molecular building block alpha beta-tubulin are established drug targets in a variety of cancers,(6,7) we still lack sufficient knowledge of the biochemistry of parasite tubulins to exploit the structural divergence between parasite and human tubulins. For example, it remains to be determined whether compounds of interest can specifically target parasite microtubules without affecting the host cell cytoskeleton. Such mechanistic insights have been limited by the lack of functional parasite tubulin. In this study, we report the purification and characterization of tubulin from Plasmodium falciparum, the causative agent of malaria. We show that the highly purified tubulin is fully functional, as it efficiently assembles into microtubules with specific parameters of dynamic instability. There is a high degree of amino-acid conservation between human and P. falciparum alpha- and beta-tubulin, sharing approximately 83.7% and 88.5% identity, respectively. However, Plasmodium tubulin is more similar to plant than to mammalian tubulin, raising the possibility of identifying compounds that would selectively disrupt parasite microtubules without affecting the host cell cytoskeleton. As a proof of principle, we describe two compounds that exhibit selective toxicity toward parasite tubulin. Thus, the ability to specifically disrupt protozoan microtubule growth without affecting human microtubules provides an exciting opportunity for the development of novel antimalarials.
引用
收藏
页码:919 / +
页数:15
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