A De novo Peptide from a High Throughput Peptide Library Blocks Myosin A -MTIP Complex Formation inPlasmodium falciparum

被引:7
作者
Anam, Zill e [1 ]
Joshi, Nishant [2 ]
Gupta, Sakshi [3 ]
Yadav, Preeti [1 ]
Chaurasiya, Ayushi [1 ]
Kahlon, Amandeep Kaur [1 ]
Kaushik, Shikha [1 ]
Munde, Manoj [3 ]
Ranganathan, Anand [1 ]
Singh, Shailja [1 ]
机构
[1] Jawaharlal Nehru Univ, Special Ctr Mol Med, New Delhi 110067, India
[2] Shiv Nadar Univ, Sch Nat Sci, Dept Life Sci, Greater Noida 201304, Uttar Pradesh, India
[3] Jawaharlal Nehru Univ, Sch Phys Sci, New Delhi 110067, India
关键词
malaria; peptide inhibitor; myosin A; myosin A tail interacting protein (MTIP); MALARIA PARASITE INVASION; INTERACTING PROTEIN MTIP; HOST-CELL INVASION; PLASMODIUM-FALCIPARUM; ERYTHROCYTE INVASION; TAIL; MEROZOITE; BINDING; ASSOCIATION; ACTIVATION;
D O I
10.3390/ijms21176158
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
Apicomplexan parasites, through their motor machinery, produce the required propulsive force critical for host cell-entry. The conserved components of this so-called glideosome machinery are myosin A and myosin A Tail Interacting Protein (MTIP). MTIP tethers myosin A to the inner membrane complex of the parasite through 20 amino acid-long C-terminal end of myosin A that makes direct contacts with MTIP, allowing the invasion ofPlasmodium falciparumin erythrocytes. Here, we discovered through screening a peptide library, a de-novo peptide ZA1 that binds the myosin A tail domain. We demonstrated that ZA1 bound strongly to myosin A tail and was able to disrupt the native myosin A tail MTIP complex both in vitro and in vivo. We then showed that a shortened peptide derived from ZA1, named ZA1S, was able to bind myosin A and block parasite invasion. Overall, our study identified a novel anti-malarial peptide that could be used in combination with other antimalarials for blocking the invasion ofPlasmodium falciparum.
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页码:1 / 17
页数:17
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