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Mattia D. Pizzagalli

ORCID: 0000-0003-0074-1039
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About
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A5056326209
Research Areas
  • Protein Degradation and Inhibitors
  • Epigenetics and DNA Methylation
  • Molecular Sensors and Ion Detection
  • Drug Transport and Resistance Mechanisms
  • interferon and immune responses
  • Immune Response and Inflammation
  • Amino Acid Enzymes and Metabolism
  • Neutrophil, Myeloperoxidase and Oxidative Mechanisms
  • Trace Elements in Health
  • Histone Deacetylase Inhibitors Research
  • Advanced MRI Techniques and Applications
  • Cancer-related gene regulation
  • Redox biology and oxidative stress
  • Advanced Neuroimaging Techniques and Applications
  • HIV/AIDS drug development and treatment
  • Mitochondrial Function and Pathology
  • Glioma Diagnosis and Treatment

Brown University
 2024

Rhode Island Hospital
 2024

CeMM Research Center for Molecular Medicine
 2020

Austrian Academy of Sciences
 2020

Boston College
 2017

 TASL is the SLC15A4-associated adaptor for IRF5 activation by TLR7–9
OPENALEX - Publications 
Leonhard X. Heinz JangEun Lee Utkarsh Kapoor Felix Kartnig Vitaly Sedlyarov and 17 more Κωνσταντίνος Παπακώστας Adrián César‐Razquin Patrick Essletzbichler Ulrich Goldmann Adrijana Stefanovic Johannes W. Bigenzahn Stefania Scorzoni Mattia D. Pizzagalli Ariel Bensimon André C. Müller Frederick J. King Jun Li Enrico Girardi M. Lamine Mbow Charles E. Whitehurst Manuele Rebsamen Giulio Superti‐Furga

10.1038/s41586-020-2282-0 article EN Nature 2020-05-13
 Targeted Degradation of SLC Transporters Reveals Amenability of Multi-Pass Transmembrane Proteins to Ligand-Induced Proteolysis
OPENALEX - Publications 
Ariel Bensimon Mattia D. Pizzagalli Felix Kartnig Vojtech Dvorak Patrick Essletzbichler and 2 more Georg Winter Giulio Superti‐Furga

With more than 450 members, the solute carrier (SLC) group of proteins represents largest class transporters encoded in human genome. Their several-pass transmembrane domain structure and hydrophobicity contribute to orphan status many SLCs, devoid known cargos or chemical inhibitors. We report that SLC belonging different families subcellular compartments are amenable induced degradation by heterobifunctional ligands. Engineering endogenous alleles via tag (dTAG) technology enabled control...

10.1016/j.chembiol.2020.04.003 article EN cc-by-nc-nd Cell chemical biology 2020-05-07
 Identifying Functional Cysteine Residues in the Mitochondria
OPENALEX - Publications 
Daniel W. Bak Mattia D. Pizzagalli Eranthie Weerapana

The mitochondria are dynamic organelles that regulate oxidative metabolism and mediate cellular redox homeostasis. Proteins within the exposed to large fluxes in surrounding environment. In particular, cysteine residues mitochondrial proteins sense respond these changes through modifications of thiol group. These result a loss reactivity, which can be monitored using cysteine-reactive chemical probes quantitative mass spectrometry (MS). Analysis cell lysates treated with enable...

10.1021/acschembio.6b01074 article EN ACS Chemical Biology 2017-02-03
 Heterochromatin spreading in cancer cells through HDAC7 mediated histone H3.3 landscape reprogramming
OPENALEX - Publications 
Ola Hassan Mattia D. Pizzagalli Owen P. Leary John P. Zepecki Adrianne Corseri and 9 more Laura Jinxuan Wu Shiven Sasipalli Daniel J. Lee Larry Hayward Lily Tran Eduardo Fajardo András Fiser David Karambizi Nikos Tapinos

Class IIa histone deacetylases (HDACs) are a family of enzymes with minimal deacetylase activity but can function as multi-protein interaction hubs. Here we demonstrate the expression HDAC7, HDAC member, in glioblastoma tumor tissue from 84 patients, patient-derived glioma stem cells (GSCs) six and pediatric diffuse pontine (DIPG) three patients. HDAC7 binds to Histone H3.3 interacts HIRA on chromatin. Targeted downregulation subtype-specific siRNA inhibits while increasing association DAXX...

10.1101/2024.03.12.584656 preprint EN bioRxiv (Cold Spring Harbor Laboratory) 2024-03-14
 Tumor-Associated Tractography Derived from High-Angular-Resolution Q-Space MRI May Predict Patterns of Cellular Invasion in Glioblastoma
OPENALEX - Publications 
Owen P. Leary John P. Zepecki Mattia D. Pizzagalli Steven A. Toms David D. Liu and 9 more Yusuke Suita Yao Ding Jihong Wang Renjie He Caroline Chung Clifton D. Fuller Jerrold L. Boxerman Nikos Tapinos Richard J. Gilbert

Background: The invasion of glioblastoma cells beyond the visible tumor margin depicted by conventional neuroimaging is believed to mediate recurrence and predict poor survival. Radiomic biomarkers that are associated with direction extent infiltration are, however, non-existent. Methods: Patients from a single center newly diagnosed (n = 7) underwent preoperative Q-space magnetic resonance imaging (QSI; 3T, 64 gradient directions, b 1000 s/mm2) between 2018 2019. Tumors were manually...

10.3390/cancers16213669 article EN Cancers 2024-10-30
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