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12 research outputs found

Autophagy in major human diseases

Autophagy is a core molecular pathway for the preservation of cellular and organismal homeostasis. Pharmacological and genetic interventions impairing autophagy responses promote or aggravate disease in a plethora of experimental models. Consistently, mutations in autophagy-related processes cause severe human pathologies. Here, we review and discuss preclinical data linking autophagy dysfunction to the pathogenesis of major human disorders including cancer as well as cardiovascular, neurodegenerative, metabolic, pulmonary, renal, infectious, musculoskeletal, and ocular disorders

MDC Repository

SMAC

Author: Amaravadi R.K.
Fetterly G.J.
Krajewska M.
Runckel K.L.
Schimmer A.D.
Tamm I.
Wang S.G.
Publication venue: 'Wiley'
Publication date
Field of study

Crossref

Repopulation of Ovarian Cancer Cells after Chemotherapy

Author: Amaravadi R.K.
Coley H.M.
Curley M.D.
Freeburg E.M.
Licun W.
Lu Z.
Ohtsu T.
Ross A.A.
Rowinsky E.K.
Schmitt C.A.
Tentes A.A.
Publication venue: 'SAGE Publications'
Publication date
Field of study

Crossref

Response, Resistance Mechanisms, and Biomarkers for Radiation and Immune Checkpoint Blockade

Author: Amaravadi R.K
Benci J.L
Christina T.S.V
Feldman M.D
Gangadhar T.C
Hahn S.M
Ishwaran H
Maity A
Mick R
Minn A.J
Odorizzi P.M
Pauken K.E
Pryma D.A
Rech A.J
Rengan R
Schuchter L.M
Stelekati E
Vonderheide R.H
Wherry E.J
Xu X
Publication venue: Elsevier Inc
Publication date: 01/11/2015
Field of study

Crossref

University of Miami: Scholarship Miami

Screening anti-tumor constituents from <em>Potamogeton crispus</em> for potential utilisation of constructed wetland plant resources

Author: A.A. Obermeyer
A.H. Wyllie
C.H. Yam
D. Ren
D. Ren
D.J. Newman
Du
Feng
G. Majno
G.A. Cordell
H. Kunii
H.B. Wang
J. Chi
J. Vymazal
J. Wu
Liu
M. Pagano
M.B. Hafez
M.F. Balandrin
M.P. Ciria
N. Bendris
P. Waridel
P. Waridel
R.K. Amaravadi
S.R. Jing
T.P. Albright
Wang
Y.X. Jian
Z. Darzynkiewicz
Zhang
Publication venue: 'Royal Irish Academy'
Publication date: 01/01/2014
Field of study

Crossref

Peroxynitrite in the tumor microenvironment changes the profile of antigens allowing escape from cancer immunotherapy.

Author: Altiok S.
Amaravadi R.K.
Antonia S.
Beer T.
Celis E.
Donthireddy L.R.
Ferrone S.
Gabrilovich D.I.
Hembach P.
Ignatov D.
Karakousis G.C.
Laufer T.
Maby-El Hajjami H.
Marvel D.
Meyer C.
Mitchell T.C.
Montaner L.J.
Mostafa A.
Pisarev V.
Sanseviero E.
Schuchter L.M.
Speicher D.W.
Speiser D.E.
Tang H.Y.
Tcyganov E.N.
Tsyganova S.
Xu W.
Xu X.
Yuan Z.
Zhang Q.
Zheng C.
Publication venue: 'Elsevier BV'
Publication date: 10/10/2022
Field of study

Cancer immunotherapy often depends on recognition of peptide epitopes by cytotoxic T lymphocytes (CTLs). The tumor microenvironment (TME) is enriched for peroxynitrite (PNT), a potent oxidant produced by infiltrating myeloid cells and some tumor cells. We demonstrate that PNT alters the profile of MHC class I bound peptides presented on tumor cells. Only CTLs specific for PNT-resistant peptides have a strong antitumor effect in vivo, whereas CTLs specific for PNT-sensitive peptides are not effective. Therapeutic targeting of PNT in mice reduces resistance of tumor cells to CTLs. Melanoma patients with low PNT activity in their tumors demonstrate a better clinical response to immunotherapy than patients with high PNT activity. Our data suggest that intratumoral PNT activity should be considered for the design of neoantigen-based therapy and also may be an important immunotherapeutic target

Serveur académique lausannois

Alternative temozolomide dosing regimens and novel combinations for the treatment of advanced metastatic melanoma

Crossref