Affiliation:
1. Malaria and Vector Research Group (MVRG), Biotechnology Research Center (BRC), Pasteur Institute of Iran, Tehran, Iran
Abstract
ABSTRACT
Malaria is one of the most important infectious diseases in the world, and it has many economic and social impacts on populations, especially in poor countries. Transmission-blocking vaccines (TBVs) are valuable tools for malaria eradication. A study on
Anopheles gambiae
revealed that polyclonal antibodies to carboxypeptidase B1 of
A. gambiae
can block sexual parasite development in the mosquito midgut. Hence, it was introduced as a TBV target in regions where
A. gambiae
is the main malaria vector. However, in Iran and neighboring countries as far as China, the main malaria vector is
Anopheles stephensi
. Also, the genome of this organism has not been sequenced yet. Therefore, in this study, carboxypeptidase B1 of
A. stephensi
was characterized by genomic and proteomic approaches. Furthermore, its expression pattern after ingestion of
Plasmodium falciparum
gametocytes and the effect of anti-CPBAs1 antibodies on sexual parasite development were evaluated. Our results revealed that the
cpbAs1
expression level was increased after ingestion of the mature gametocytes of
P. falciparum
and that anti-CPBAs1 directed antibodies could significantly reduce the mosquito infection rate in the test group compared with the control group. Therefore, according to our findings and with respect to the high similarity of carboxypeptidase enzymes between the two main malaria vectors in Africa (
A. gambiae
) and Asia (
A. stephensi
) and the presence of other sympatric vectors, CPBAs1 could be introduced as a TBV candidate in regions where
A. stephensi
is the main malaria vector, and this will broaden the scope for the potential wider application of CPBAs1 antigen homologs/orthologs.
Publisher
American Society for Microbiology
Subject
Infectious Diseases,Immunology,Microbiology,Parasitology
Cited by
38 articles.
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