Publications by authors named "I Draskovic"

The innovative design of a triarylborane (TB)-dye with one NMe-alkylated (propargylated) group and one NMe group yielded a system that is both an NMe π-donor and an inductive NMe-alkyl cationic acceptor. Consequently, the new TB-dye was highly sensitive to a "click" reaction with an azide-substituted lysine side chain (yielding TB-lysine), resulting in a bathochromic shift of emission of 100 nm. In addition, fluorene attached to the lysine C-terminus showed FRET with the TB-chromophore, also sensitive to interactions with targets.

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The low seroprevalent human adenovirus type 26 (HAdV26)-based vaccine vector was the first adenovirus-based vector to receive marketing authorization from European Commission. HAdV26-based vaccine vectors induce durable humoral and cellular immune responses and, as such, represent a highly valuable tool for fighting infectious diseases. Despite well-described immunogenicity in vivo, the basic biology of HAdV26 still needs some refinement.

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Dyskeratosis congenita is a cancer-prone inherited bone marrow failure syndrome caused by telomere dysfunction. A mouse model recently suggested that p53 regulates telomere metabolism, but the clinical relevance of this finding remained uncertain. Here, a germline missense mutation of , a negative regulator of p53, was found in a family with features suggestive of dyskeratosis congenita, e.

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G-quadruplex ligands exert their antiproliferative effects through telomere-dependent and telomere-independent mechanisms, but the inter-relationships among autophagy, cell growth arrest and cell death induced by these ligands remain largely unexplored. Here, we demonstrate that the G-quadruplex ligand 20A causes growth arrest of cancer cells in culture and in a HeLa cell xenografted mouse model. This response is associated with the induction of senescence and apoptosis.

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Article Synopsis
  • Pheochromocytomas and paragangliomas (PPGLs) are rare neuroendocrine tumors, with about 20% having the potential to metastasize, especially those with specific mutations.
  • This study investigated how immortalization processes, like telomerase activation and alternative lengthening of telomeres (ALT), relate to the likelihood of metastatic progression in 200 tumors.
  • Findings indicated that only 18.5% of tumors were immortalized, with telomerase activation linked to worse outcomes, suggesting that analyzing these mechanisms could help identify high-risk metastatic PPGLs.
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