, 2010) Considering that the Drosophila P0 protein has DNase and

, 2010). Considering that the Drosophila P0 protein has DNase and endonuclease activities (Yacoub et al., 1996), it is reasonable to suspect that phosphorylated C. cucullus p33 may be involved in such macronuclear events. Furthermore, the P0 protein may play a role in regulating metabolism during pupal diapause of the flesh fly (Craig & Denlinger, 2000). The C. cucullus p33 may be involved in

the regulation of metabolic activity directly FDA approved Drug Library purchase or through gene expression, because mitochondrial membrane potential disappeared in the early stage of encystment (Funatani et al., 2010). It is also likely that C. cucullus p33 plays a role in the regulation of encystment-specific gene expression, as was reported in Drosophila. In fact, the expression of encystment-specific proteins in C. cucullus was recently found to be regulated at the Selleckchem MK1775 transcriptional level (in preparation). In many organisms, the ribosomal S5 protein consists of 190–230 amino acid residues (blast Search) and its free form is phosphoprotein (Matragkou et al., 2009). Taking into account that in mammalian cells, the ribosomal S5 protein has been reported to

be involved in the arrest of cell cycle and the initiation of differentiation (Matragkou et al., 2008),and the p24 must also be involved in the cell cycle arrest and differentiation into resting cyst form in C. cucullus. “
“A large number of novel bioactive compounds were discovered from microbial secondary metabolites based on the traditional bioactivity screenings. Recent fermentation studies indicated that the crude extract of marine Streptomyces sp. W007 possessed great potential in agricultural fungal disease control against Phomopsis asparagi, Polystigma deformans, Cladosporium cucumerinum, Monilinia fructicola, and Colletotrichum lagenarium. To further evaluate the biosynthetic potential of secondary metabolites, we sequenced the genome of Streptomyces sp. W007 and analyzed the identifiable secondary metabolite gene clusters. Moreover, one gene

cluster with type II PKS implied the possibility of Streptomyces sp. W007 to produce aromatic polyketide of angucyclinone antibiotics. Therefore, two novel compounds, 3-hydroxy-1-keto-3-methyl-8-methoxy-1,2,3,4-tetrahydro-benz[α]anthracene and kiamycin with Casein kinase 1 potent cytotoxicities against human cancer cell lines, were isolated from the culture broth of Streptomyces sp. W007. In addition, other four known angucyclinone antibiotics were obtained. The gene cluster for these angucyclinone antibiotics could be assigned to 20 genes. This work provides powerful evidence for the interplay between genomic analysis and traditional natural product isolation research. Microbial natural products are an important source of new drugs (Solanki et al., 2008). Among the producers of commercially important metabolites, actinomycetes have proven to be a prolific source with a surprisingly small group of taxa accounting for the vast majority of compounds.

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