Presence of chitinase and beta-N-acetylglucosaminidase in the Aedes aegypti A chitinolytic system involving peritrophic matrix formation and degradation
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Filho, BPD
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机构:Ctr Pesquisas Rene Rachou Fiocruz, Lab Med Entomol, Fundacao Oswaldo Cruz, BR-30190002 Belo Horizonte, MG, Brazil
Filho, BPD
Lemos, FJA
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机构:Ctr Pesquisas Rene Rachou Fiocruz, Lab Med Entomol, Fundacao Oswaldo Cruz, BR-30190002 Belo Horizonte, MG, Brazil
Lemos, FJA
Secundino, NFC
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机构:Ctr Pesquisas Rene Rachou Fiocruz, Lab Med Entomol, Fundacao Oswaldo Cruz, BR-30190002 Belo Horizonte, MG, Brazil
Secundino, NFC
Páscoa, V
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机构:Ctr Pesquisas Rene Rachou Fiocruz, Lab Med Entomol, Fundacao Oswaldo Cruz, BR-30190002 Belo Horizonte, MG, Brazil
Páscoa, V
Pereira, ST
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机构:Ctr Pesquisas Rene Rachou Fiocruz, Lab Med Entomol, Fundacao Oswaldo Cruz, BR-30190002 Belo Horizonte, MG, Brazil
Measurement of the hydrolysis of specific fluorogenic substrates by spectrophotometry as well as the substrate activity-SDS-PAGE gel analysis of the chitinolytic activity in Aedes aegypti guts showed that both chitinase and P-N-acetylglucosaminidase are present and physiologically active. Both enzymes were present even in guts from unfed insects, but the activities increased rapidly after feeding on blood or an artificial protein-free diet. Chitinase activity was predominantly of the 'endo'-type, reaching its maximum activity at 36 h and then declining to very low levels after the degradation of the peritrophic matrix (PM). Chitinase assay in gels after SDS-PAGE was a very sensitive method that allowed us to detect two chitinases with distinct molecular weights in the mosquito gut. Hydrolysis of a chitinase-specific substrate by chitinolytic activities in the mosquito guts was inhibited by allosamidin, a potent chitinase inhibitor. Allosamidin treatment led to the formation of an atypical thick PM, while the addition of exogenous chitinase completely blocked its formation. This chitinolytic system appears to operate both on the formation and degradation of the PM. Since the PM is involved in pathogen invasion, these results are important in facilitating a search for mechanisms that can block pathogen development in the mosquito vector. (C) 2002 Elsevier Science Ltd. All rights reserved.
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NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,DEPT EXPTL THERAPEUT,666 ELM ST,BUFFALO,NY 14263NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,DEPT EXPTL THERAPEUT,666 ELM ST,BUFFALO,NY 14263
WOYNAROWSKA, B
WIKIEL, H
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NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,DEPT EXPTL THERAPEUT,666 ELM ST,BUFFALO,NY 14263NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,DEPT EXPTL THERAPEUT,666 ELM ST,BUFFALO,NY 14263
WIKIEL, H
BERNACKI, RJ
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NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,DEPT EXPTL THERAPEUT,666 ELM ST,BUFFALO,NY 14263NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,DEPT EXPTL THERAPEUT,666 ELM ST,BUFFALO,NY 14263
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NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,BUFFALO,NY 14263NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,BUFFALO,NY 14263
WOYNAROWSKA, B
BERNACKI, RJ
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NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,BUFFALO,NY 14263NEW YORK STATE DEPT HLTH,ROSWELL PK MEM INST,GRACE CANC DRUG CTR,BUFFALO,NY 14263
BERNACKI, RJ
PROCEEDINGS OF THE AMERICAN ASSOCIATION FOR CANCER RESEARCH,
1988,
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