Publications by authors named "Ivanildce C Ireno"

Synthetic lethal interactions between poly (ADP-ribose) polymerase (PARP) and homologous recombination (HR) repair pathways have been exploited for the development of novel mono- and combination cancer therapies. The tumor suppressor p53 was demonstrated to exhibit indirect and direct regulatory activities in DNA repair, particularly in DNA double-strand break (DSB)-induced and replication-associated HR. In this study, we tested a potential influence of the p53 status on the response to PARP inhibition, which is known to cause replication stress.

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Article Synopsis
  • In vitro genotoxicity tests often lack specificity, especially in mammalian cell assays, prompting the development of a new fluorescence-based method in living human cells.
  • This method measures DNA recombination events due to DNA damage, utilizing an engineered DNA substrate from the human genome to improve sensitivity when screening different cell types.
  • The results showed that the assay effectively detects genotoxic carcinogens with over 85% sensitivity and 90% specificity, distinguishing true positives from false positives, and even identifies compounds needing metabolic activation for carcinogenicity through testing with cyclophosphamide.
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Expression of BCR-ABL oncoprotein in chronic myeloid leukemia (CML) promotes neoplastic transformation of hematopoietic stem cells through modulation of diverse pathways. CML is a multistep disease, which evolves as a chronic phase and progresses to blast crisis. This progression has been associated with the appearance and accumulation of new cytogenetic anomalies and mutations.

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The systematic investigation of the peptidic composition of the skin secretion of Phasmahyla jandaia, a phyllomedusine anuran endemic to the southern region of the Espinhaço range in Brazil, is herein reported. By means of de novo interpretation of tandem mass spectrometric data, Edman N-terminal sequencing and similarity searches, 57 peptides - including phylloseptins, dermaseptins stricto sensu, dermatoxins, hyposins, tryptophyllins, caerulein-related, bradykinin-related, bradykinin potentiating, tyrosine-rich, and opioid peptides - were sequenced. Moreover, five peptide families without significant similarity to other known molecules were verified.

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