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The peptidases of Trypanosoma cruzi: Digestive enzymes, virulence factors, and mediators of autophagy and programmed cell death
Authors:Vanina E. AlvarezGabriela T. Niemirowicz  Juan J. Cazzulo
Affiliation:
  • Instituto de Investigaciones Biotecnológicas (IIB-INTECH, Universidad Nacional de San Martín-CONICET). Avenida General Paz 5445, 1650 San Martín, Buenos Aires, Argentina
  • Abstract:Trypanosoma cruzi, the agent of the American Trypanosomiasis, Chagas disease, contains cysteine, serine, threonine, aspartyl and metallo peptidases. The most abundant among these enzymes is cruzipain, a cysteine proteinase expressed as a mixture of isoforms, some of them membrane-bound. The enzyme is an immunodominant antigen in human chronic Chagas disease and seems to be important in the host/parasite relationship. Inhibitors of cruzipain kill the parasite and cure infected mice, thus validating the enzyme as a very promising target for the development of new drugs against the disease. In addition, a 30 kDa cathepsin B-like enzyme, two metacaspases and two autophagins have been described. Serine peptidases described in the parasite include oligopeptidase B, a member of the prolyl oligopeptidase family involved in Ca2+-signaling during mammalian cell invasion; a prolyl endopeptidase (Tc80), against which inhibitors are being developed, and a lysosomal serine carboxypeptidase. Metallopeptidases homologous to the gp63 of Leishmania spp. are present, as well as two metallocarboxypeptidases belonging to the M32 family, previously found only in prokaryotes. The proteasome has properties similar to those of other eukaryotes, and its inhibition by lactacystin blocks some differentiation steps in the life cycle of the parasite. This article is part of a Special Issue entitled: Proteolysis 50 years after the discovery of lysosome.
    Keywords:CPs, cysteine proteinases   SPs, serine proteinases   MPs, metalloproteinases   APs, aspartyl proteinases   20S and 26S proteasome: proteasome oligomers with a sedimentation coefficient of 20S and 26S, respectively   Z, N-benzyloxycarbonyl   NHMec, amidomethyl coumarine   E-64, trans-epoxy succinyl amido (4-guanidino) butane   TLCK, N-? α-tosyl-lysyl-chloromethylketone   MHC, major histocompatibility complex   C-T, C-terminal domain of cruzipain   Boc, N-t-butyloxycarbonyl   pNA, p-nitroanilide   PCR, polymerase chain reaction   gp63, Leishmania surface proteinase (leishmanolysin)   POP Tc80, prolylendopeptidase Tc80 (collagenase)   TcSCP, T. cruzi serine carboxypeptidase   TcMCP-1 and TcMCP-2, T. cruzi metallocarboxypeptidase   BbCI, Bauhinia bauhinioides cysteine protease inhibitor   PCD, programmed cell death   PE, phosphatidylethanolamine
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