PMID- 30894212
OWN - NLM
STAT- MEDLINE
DCOM- 20200616
LR  - 20201023
IS  - 2051-1426 (Electronic)
IS  - 2051-1426 (Linking)
VI  - 7
IP  - 1
DP  - 2019 Mar 20
TI  - Phase 1/2 study of epacadostat in combination with ipilimumab in patients with 
      unresectable or metastatic melanoma.
PG  - 80
LID - 10.1186/s40425-019-0562-8 [doi]
LID - 80
AB  - BACKGROUND: Epacadostat is a potent inhibitor of the immunosuppressive 
      indoleamine 2,3-dioxygenase 1 (IDO1) enzyme. We present phase 1 results from a 
      phase 1/2 clinical study of epacadostat in combination with ipilimumab, an 
      anti-cytotoxic T-lymphocyte-associated protein 4 antibody, in advanced melanoma 
      (NCT01604889). METHODS: Only the phase 1, open-label portion of the study was 
      conducted, per the sponsor's decision to terminate the study early based on the 
      changing melanoma treatment landscape favoring exploration of programmed cell 
      death protein 1 (PD-1)/PD-ligand 1 inhibitor-based combination strategies. Such 
      decision was not related to the safety of epacadostat plus ipilimumab. Patients 
      received oral epacadostat (25, 50, 100, or 300 mg twice daily [BID]; 75 mg daily 
      [50 mg AM, 25 mg PM]; or 50 mg BID intermittent [2 weeks on/1 week off]) plus 
      intravenous ipilimumab 3 mg/kg every 3 weeks. RESULTS: Fifty patients received >/=1 
      dose of epacadostat. As of January 20, 2017, 2 patients completed treatment and 
      48 discontinued, primarily because of adverse events (AEs) and disease 
      progression (n = 20 each). Dose-limiting toxicities occurred in 11 patients 
      (n = 1 each with epacadostat 25 mg BID, 50 mg BID intermittent, 75 mg daily; 
      n = 4 each with epacadostat 50 mg BID, 300 mg BID). The most common 
      immune-related treatment-emergent AEs included rash (50%), alanine 
      aminotransferase elevation (28%), pruritus (28%), aspartate aminotransferase 
      elevation (24%), and hypothyroidism (10%). Among immunotherapy-naive patients 
      (n = 39), the objective response rate was 26% by immune-related response criteria 
      and 23% by Response Evaluation Criteria in Solid Tumors version 1.1. No objective 
      response was seen in the 11 patients who received prior immunotherapy. 
      Epacadostat exposure was dose proportional, with clinically significant IDO1 
      inhibition at doses >/=25 mg BID. CONCLUSIONS: When combined with ipilimumab, 
      epacadostat </=50 mg BID demonstrated clinical and pharmacologic activity and was 
      generally well tolerated in patients with advanced melanoma. TRIAL REGISTRATION: 
      ClinicalTrials.gov identifier, NCT01604889 . Registration date, May 9, 2012, 
      retrospectively registered.
FAU - Gibney, Geoffrey T
AU  - Gibney GT
AD  - Donald A. Adam Melanoma and Skin Cancer Research Center of Excellence, Moffitt 
      Cancer Center, 12902 Magnolia Drive, Tampa, FL, USA. 
      geoffrey.t.gibney@gunet.georgetown.edu.
AD  - Present Address: Lombardi Comprehensive Cancer Center, Medstar-Georgetown 
      University Hospital, 3800 Reservoir Road NW, Podium A, Washington, DC, 20007, 
      USA. geoffrey.t.gibney@gunet.georgetown.edu.
FAU - Hamid, Omid
AU  - Hamid O
AD  - Melanoma and Skin Cancers Center, The Angeles Clinic and Research Institute, 
      11818 Wilshire Blvd, Suite #200, Los Angeles, CA, USA.
FAU - Lutzky, Jose
AU  - Lutzky J
AD  - Division of Hematology & Oncology, Mount Sinai Medical Center, 4306 Alton Rd, 
      Miami Beach, FL, USA.
FAU - Olszanski, Anthony J
AU  - Olszanski AJ
AD  - Department of Hematology/Oncology, Fox Chase Cancer Center, 333 Cottman Ave, 
      Philadelphia, PA, USA.
FAU - Mitchell, Tara C
AU  - Mitchell TC
AD  - Division of Hematology Oncology, Abramson Cancer Center, Hospital of the 
      University of Pennsylvania, 3400 Civic Center Blvd, Philadelphia, PA, USA.
FAU - Gajewski, Thomas F
AU  - Gajewski TF
AD  - Department of Hematology/Oncology, University of Chicago, 5841 S Maryland Ave, 
      MC2115, Chicago, IL, USA.
FAU - Chmielowski, Bartosz
AU  - Chmielowski B
AD  - Jonsson Comprehensive Medical Center, University of California, Los Angeles, 
      10945 Le Conte Ave #2339, Los Angeles, CA, USA.
FAU - Hanks, Brent A
AU  - Hanks BA
AD  - Department of Medicine, Duke University Medical Center, 20 Duke Medicine Cir, 
      Durham, NC, USA.
FAU - Zhao, Yufan
AU  - Zhao Y
AD  - Incyte Corporation, 1801 Augustine Cutoff, Wilmington, DE, USA.
FAU - Newton, Robert C
AU  - Newton RC
AD  - Incyte Corporation, 1801 Augustine Cutoff, Wilmington, DE, USA.
FAU - Maleski, Janet
AU  - Maleski J
AD  - Incyte Corporation, 1801 Augustine Cutoff, Wilmington, DE, USA.
FAU - Leopold, Lance
AU  - Leopold L
AD  - Incyte Corporation, 1801 Augustine Cutoff, Wilmington, DE, USA.
FAU - Weber, Jeffrey S
AU  - Weber JS
AD  - Donald A. Adam Melanoma and Skin Cancer Research Center of Excellence, Moffitt 
      Cancer Center, 12902 Magnolia Drive, Tampa, FL, USA.
AD  - Present Address: Laura and Isaac Perlmutter Cancer Center, NYU Langone Medical 
      Center, New York, NY, USA.
LA  - eng
SI  - ClinicalTrials.gov/NCT01604889
GR  - K08 CA191063/CA/NCI NIH HHS/United States
PT  - Clinical Trial, Phase I
PT  - Clinical Trial, Phase II
PT  - Journal Article
PT  - Research Support, Non-U.S. Gov't
DEP - 20190320
PL  - England
TA  - J Immunother Cancer
JT  - Journal for immunotherapy of cancer
JID - 101620585
RN  - 0 (Ipilimumab)
RN  - 0 (Oximes)
RN  - 0 (Sulfonamides)
RN  - 71596A9R13 (epacadostat)
SB  - IM
MH  - Adult
MH  - Aged
MH  - Aged, 80 and over
MH  - Antineoplastic Combined Chemotherapy Protocols/*administration & dosage/adverse 
      effects
MH  - Drug Administration Schedule
MH  - Female
MH  - Humans
MH  - Ipilimumab/*administration & dosage/adverse effects
MH  - Male
MH  - Melanoma/*drug therapy
MH  - Middle Aged
MH  - Neoplasm Metastasis
MH  - Oximes/*administration & dosage/adverse effects
MH  - Sulfonamides/*administration & dosage/adverse effects
MH  - Treatment Outcome
PMC - PMC6425606
OTO - NOTNLM
OT  - Epacadostat
OT  - IDO1
OT  - Immune checkpoint inhibition
OT  - Ipilimumab
OT  - Melanoma
COIS- ETHICS APPROVAL AND CONSENT TO PARTICIPATE: This report was conducted in 
      accordance with the provisions of the Declaration of Helsinki, as described in 
      the International Council for Harmonisation Guidelines for Good Clinical 
      Practice, and was approved by the institutional review board at each 
      participating institution. All patients provided informed consent before 
      initiation of treatment. CONSENT FOR PUBLICATION: Not applicable. COMPETING 
      INTERESTS: GTG served as a consultant for Array BioPharma, Genentech, Novartis, 
      Incyte Corporation, Newlink Genetics, Jounce, and Bristol-Myers Squibb; and 
      served on a speakers bureau for Genentech. OH served consulting or advisory roles 
      with Amgen, Novartis, Roche, Bristol-Myers Squibb, and Merck; served on speakers 
      bureaus for Bristol-Myers Squibb, Genentech, Novartis, and Amgen; and received 
      research funding from AstraZeneca, Bristol-Myers Squibb, Celldex, Genentech, 
      Immunocore, Incyte, Merck, Merck Serono, MedImmune, Novartis, Pfizer, Rinat, and 
      Roche. JL served as an advisory board consultant for Bristol-Myers Squibb. AJO 
      served consulting or advisory roles with Merck, Takeda, Bristol-Myers Squibb, and 
      G1 Therapeutics; received research funding from Takeda, Immunocore, EMD Serono, 
      Amgen, Incyte, Kyowa Hakko Kirin, Lilly, Advaxis, Mirati Therapeutics, Ignyta, 
      Novartis, Pfizer, Bristol-Myers Squibb, and Kura; and received 
      travel/accommodation expenses from Takeda. TCM served consulting or advisory 
      roles with Novartis, Bristol-Myers Squibb, Merck, and Incyte; and received 
      research funding from Merck, Incyte, Bristol-Myers Squibb, and Roche. TFG has 
      received consultancy fees from Merck, Roche-Genentech, AbbVie, Bayer, Jounce, 
      Aduro, Fog Pharma, Adaptimmune, FivePrime, and Sanofi; has received research 
      support from Roche-Genentech, Bristol-Myers Squibb, Merck, Incyte, Seattle 
      Genetics, Celldex, Ono, Evelo, Bayer, and Aduro; has intellectual 
      property/licensing agreements with Aduro, Evelo, and Bristol-Myers Squibb; and is 
      a cofounder/shareholder with Jounce. BC has nothing to disclose. BAH received 
      research funding from Merck, OncoMed Pharmaceuticals, MedPacto Inc., 
      GlaxoSmithKline, AstraZeneca, D3 A*STAR, and Tempest; served consulting or 
      advisory roles for G1 Therapeutics and FujiFilm Pharmaceuticals; and served on 
      speakers bureaus for CE Concepts and Merck. YZ was an employee and stockholder of 
      Incyte Corporation at the time of data analysis. RCN, JM, and LL are employees 
      and stockholders of Incyte Corporation. JSW owns equity in Biond, Altor, and 
      CytomX; is named on patents for Biodesix (PD-1 biomarker) and Moffitt (CTLA-4 
      biomarker; neither of which were used in the current work); and has received 
      consulting fees for advisory boards for Bristol-Myers Squibb, GlaxoSmithKline, 
      Merck, Novartis, Incyte Corporation, Genentech, AstraZeneca, Celldex, Sellas, 
      CytomX, EMD Serono, and Pfizer. PUBLISHER'S NOTE: Springer Nature remains neutral 
      with regard to jurisdictional claims in published maps and institutional 
      affiliations.
EDAT- 2019/03/22 06:00
MHDA- 2020/06/17 06:00
PMCR- 2019/03/20
CRDT- 2019/03/22 06:00
PHST- 2018/12/26 00:00 [received]
PHST- 2019/03/11 00:00 [accepted]
PHST- 2019/03/22 06:00 [entrez]
PHST- 2019/03/22 06:00 [pubmed]
PHST- 2020/06/17 06:00 [medline]
PHST- 2019/03/20 00:00 [pmc-release]
AID - 10.1186/s40425-019-0562-8 [pii]
AID - 562 [pii]
AID - 10.1186/s40425-019-0562-8 [doi]
PST - epublish
SO  - J Immunother Cancer. 2019 Mar 20;7(1):80. doi: 10.1186/s40425-019-0562-8.