Sandro Cosconati

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Sandro Cosconati

Sandro Cosconati

@scoscona

Caserta, Campania Beigetreten Eylül 2009
490 Folgt212 Follower
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ESMEC
ESMEC@esmecurbino·
ESMEC 2025 URBINO - European School of Medicinal Chemistry: June 29 – July 3, 2025 Tentative Programme Available and REGISTRATION is nor OPEN! For all the info: esmec.eu We are waiting for you in Urbino! @DCFSCI @EuroMedChem @YoungSciNet @SciGiovani
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Biology+AI Daily
Biology+AI Daily@BiologyAIDaily·
Discovering Dually Active Anti-cancer Compounds with a Hybrid AI-structure-based Approach @JCIM_JCTC 1/ In this study, a novel hybrid AI-structure-based approach was developed to identify compounds that can target both G-quadruplex (G4) structures and the poly(ADP-ribose) polymerase (PARP1) enzyme, opening the door to innovative cancer therapies with dual action. 2/ The innovative two-step virtual screening protocol integrates machine learning and structure-based methods. PyRMD, an AI-powered tool, identifies potential PARP1 inhibitors from vast chemical libraries, then evaluates them for their G4 stabilization potential. 3/ By combining AI and structure-based screening, the study identifies four compounds with dual PARP1 inhibition and G4 stabilization activity, offering a multipronged strategy to disrupt cancer cell proliferation. 4/ The identified compounds show significant antiproliferative activity, particularly against cancer cell lines with BRCA1 mutations, suggesting the potential for targeting tumors with DNA repair deficiencies. 5/ One compound, in particular, demonstrated activity against telomerase-positive HeLa cells, hinting at its broader applicability across different cancer types, making it a versatile therapeutic candidate. 6/ This study showcases the potential of hybrid AI-driven approaches in drug discovery, emphasizing the power of combining machine learning with classical structure-based methods to develop multitarget anticancer compounds. @scoscona 📜Paper: doi.org/10.1021/acs.jc…
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EFMC
EFMC@EuroMedChem·
📣 Session 9 – Prof. Sandro COSCONATI from @unicampania is now on the stage for talk titled “From Reversible to Irreversible Peptide Inhibitors of the TRF2TRFH Recruiting Functions: a Strategy to Induce Replication Stress in Cancer Cells”. Stay tuned! 🔬💡 #EFMCISMC24 #MedChem
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Gianluca Sbardella
Gianluca Sbardella@g_sbardella·
Next talk in the peptide session at #EFMCISMC24 is given by Sandro Cosconati (@scoscona), describing his strategy to induce replication stress in cancer cells, from reversible to irreversible peptide inhibitors of the TRF2TRFH recruiting functions. @EuroMedChem @DCFSCI
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Keriann Backus
Keriann Backus@Keribackus·
Bit of good news to end the week---and a big big thank you to everyone who helped make this possible, especially all members of our lab past and present, mentors, letter writers, colleagues, friends+family.
UCLA Biological Chemistry@BC_UCLA

We are thrilled to announce that @Keribackus has been promoted to the rank of Associate Professor with tenure! We congratulate Keri on this well-deserved achievement and look forward to her lab continuing to make impactful discoveries! 👏👏🎉🍾

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Cell Chemical Biology
Cell Chemical Biology@CellChemBiol·
Online now! Irreversible inhibition of TRF2TRFH recruiting functions by a covalent cyclic peptide induces telomeric replication stress in cancer cells by Alexander Sobinoff, Salvatore Di Maro, @hildaApickett, @scoscona, et al dlvr.it/SzrGYZ #chembiol
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Sandro Cosconati
Sandro Cosconati@scoscona·
Co-treatment with the G4 stabilizing agent RHPS4 amplifies APOD53's effects on telomeric replication stress, offering a potential combination strategy for cancer treatment. The interplay between TRFH targeting peptides and replication stress inducers is explored.
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Sandro Cosconati
Sandro Cosconati@scoscona·
APOD53's impact goes beyond inhibiting TRF2; it blocks the interaction of RTEL1 and SLX4 with TRF2, inducing replication stress, DNA damage, and telomere fragility. This sets the stage for a robust telomeric DNA damage response.
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