Carmine Fedele

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Carmine Fedele

Carmine Fedele

@CarminuzzoF

Lab head, Senior Principal Scientist, Oncology/Drug discovery. tweets are my own

Cambridge, MA Katılım Ocak 2010
488 Takip Edilen401 Takipçiler
Carmine Fedele
Carmine Fedele@CarminuzzoF·
@raffcolo @HartungIngo Do you have a model to test ADC efficacy in a highly fibrotic TME? PANC CDX models usually lack clinically relevant fibrosis, so it’s unclear whether the ADC can effectively reach tumor cells in this context.
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Ingo Hartung
Ingo Hartung@HartungIngo·
If you come late enough you can even get through to the Zymeworks pan-Ras inhibitor ADC poster at #AACR26! @raffcolo
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Lucia Languino
Lucia Languino@LLanguino·
@LanguinoLu21124 Time to apply for the August 2026 Gordon Research Conference on Extracellular Vesicles: basic science discoveries, biomarker and therapeutic development. Limited number: GRC allows only 200 participants. Location: Barcelona, Spain 2026.
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Lucia Languino
Lucia Languino@LanguinoLu21124·
GRC- Extracellular Vesicles 2026
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Daniel Gerlach
Daniel Gerlach@gerlach_d·
Excited to share our recent work on the pan-KRAS inhibitors BI-2493 and BI-2865, displaying potent anti-tumor activity in tumors with #KRAS wild-type allele amplification. doi.org/10.1158/1535-7… Great team effort by team @Boehringer !
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Alice Ting
Alice Ting@aliceyting·
Could one envision a synthetic receptor technology that is fully programmable, able to detect diverse extracellular antigens – both soluble and cell-attached – and convert that recognition into a wide range of intracellular responses, from transgene expression and real-time fluorescence to modulation of innate cell behavior (excitation or inhibition of neurons, induction of cell migration, etc.)? Today we report in Nature a new technology platform that provides a step in that direction: PAGERs, for Programmable Antigen-gated G protein-coupled Engineered Receptors, convert recognition of extracellular soluble or cell-attached antigens into diverse user-selected responses. PAGERs are based on G-protein coupled receptors (GPCRs), which themselves are not structurally modular, but we were able to build in modular antigen gating by fusing an antagonist peptide to the extracellular N-terminal end, and then gating the antagonist with a fused antigen-binding nanobody.  When antigen binds, it sterically interferes with the antagonist, leading to relief of receptor inhibition. Drug or agonist can then turn on PAGER. nature.com/articles/s4158…
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Martina Parigi
Martina Parigi@parigi_martina·
Very excited to share our latest work on the uncoupling of epithelial regeneration and tumorigenesis in the gut! nature.com/articles/s4158…
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Miriam Molina Arcas
Miriam Molina Arcas@molina_arcas·
Interested on how to combine #KRAS inhibitors with immunotherapies? Check out the last paper of the #Downwardlab and @F_vanMaldegem
Febe van Maldegem@F_vanMaldegem

science.org/doi/10.1126/sc… T cells receive regulatory signals from close neighbours, through ligand-receptor interactions and cytokines. Therefore we dived into the local neighbourhoods of CD8 T cells to investigate why a lung cancer model was resistant to KRAS-G12C-i + a-PD1.

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Cancer Cell
Cancer Cell@Cancer_Cell·
Online Now: The hallmarks of cancer immune evasion dlvr.it/TFFy1H
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Michael Erb
Michael Erb@Michael_A_Erb·
Open season on FOXA1! Our paper with the Cravatt group is out today in @MolecularCell. Please check out the updated data, including a new discovery that FOXA1 ligands mirror the effects of a nearby prostate cancer mutation. authors.elsevier.com/a/1jxLO3vVUPRn… (1/2)
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Ferdinandos Skoulidis
Ferdinandos Skoulidis@FSkoulidis·
Excited to share our new study @Nature. Very grateful for the support of our collaborators, pharma and biotech partners and members of the Skoulidis and Heymach labs. Special thanks to star fellow @_hanielaraujo and @minhtruongdo. Thankful to our patients. @MDAndersonNews
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Miriam Molina Arcas
Miriam Molina Arcas@molina_arcas·
Excited to share our last paper out today in @NatureComms Led by the talented @Anastap78 #KRAS #immunotherapies #NSCLC
Julian Downward@JulianDownward

How can we extend responses to KRASG12C drugs? Out now in @NatureComms, combining Revolution Medicines’ RAS(ON) G12C-selective inhibitor with a SHP2 inhibitor and immune checkpoint blockade to study their effects on KRAS-mutant lung tumours of varying immunogenicities.

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Cancer Cell
Cancer Cell@Cancer_Cell·
Online Now: Distinct clinical outcomes and biological features of specific KRAS mutants in human pancreatic cancer dlvr.it/TCXth0
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Ryan Potts
Ryan Potts@pottslab·
New print posted from the group @Amgen. We describe VIPER-TACs that leverage viral E3 ligases for disease-specific targeted protein degradation. This concept dramatically expands he druggable space to include pan-essential proteins. 🧵 #mycompany biorxiv.org/content/10.110…
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