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Please use this identifier to cite or link to this item: https://repository.monashhealth.org/monashhealthjspui/handle/1/29145
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dc.contributor.authorWu C.-Y.en
dc.contributor.authorZhang Y.en
dc.contributor.authorLiang L.en
dc.contributor.authorWu J.en
dc.contributor.authorPaton V.en
dc.contributor.authorMillward M.en
dc.contributor.authorKeam B.en
dc.contributor.authorJameson M.en
dc.contributor.authorHou M.-M.en
dc.contributor.authorKang Y.-K.en
dc.contributor.authorMarkman B.en
dc.contributor.authorLu C.-H.en
dc.contributor.authorRau K.-M.en
dc.contributor.authorLee K.-H.en
dc.contributor.authorHorvath L.en
dc.contributor.authorFriedlander M.en
dc.contributor.authorHill A.en
dc.contributor.authorSandhu S.en
dc.contributor.authorBarlow P.en
dc.contributor.authorDesai J.en
dc.contributor.authorDeva S.en
dc.contributor.authorLee J.S.en
dc.contributor.authorLin C.-C.en
dc.contributor.authorYen C.-J.en
dc.contributor.authorChao Y.en
dc.date.accessioned2021-05-14T09:50:14Zen
dc.date.available2021-05-14T09:50:14Zen
dc.date.copyright2020en
dc.date.created20200704en
dc.date.issued2020-07-04en
dc.identifier.citationJournal for ImmunoTherapy of Cancer. 8 (1) (no pagination), 2020. Article Number: e000453. Date of Publication: 14 Jun 2020.en
dc.identifier.issn2051-1426 (electronic)en
dc.identifier.urihttps://repository.monashhealth.org/monashhealthjspui/handle/1/29145en
dc.description.abstractBackground The programmed cell death-1/programmed cell death ligand-1 (PD-1/PD-L1) axis plays a central role in suppressing antitumor immunity; axis dysregulation can be used by cancer cells to evade the immune system. Tislelizumab, an investigational monoclonal antibody with high affinity and binding specificity for PD-1, was engineered to minimize binding to Fc 3R on macrophages to limit antibody-dependent phagocytosis, a potential mechanism of resistance to anti-PD-1 therapy. The aim of this phase IA/IB study was to investigate the safety/tolerability, antitumor effects and optimal dose and schedule of tislelizumab in patients with advanced solid tumors. Methods Patients (aged >=18 years) enrolled in phase IA received intravenous tislelizumab 0.5, 2, 5 or 10 mg/kg every 2 weeks; 2 or 5 mg/kg administered every 2 weeks or every 3 weeks; or 200 mg every 3 weeks; patients in phase IB received 5 mg/kg every 3 weeks. Primary objectives were to assess tislelizumab's safety/tolerability profile by adverse event (AE) monitoring and antitumor activity using RECIST V.1.1. PD-L1 expression was assessed retrospectively with the VENTANA PD-L1 (SP263) Assay. Results Between May 2015 and October 2017, 451 patients (n=116, IA; n=335, IB) were enrolled. Fatigue (28%), nausea (25%) and decreased appetite (20%) were the most commonly reported AEs. Most AEs were grade 1-2 severity; anemia (4.9%) was the most common grade 3-4 AE. Treatment-related AEs led to discontinuation in 5.3% of patients. Grade 5 AEs were reported in 14 patients; 2 were considered related to tislelizumab. Pneumonitis (2%) and colitis (1%) were the most common serious tislelizumab-related AEs. As of May 2019, 18% of patients achieved a confirmed objective response in phase IA and 12% in phase IB; median follow-up duration was 13.6 and 7.6 months, respectively. Pharmacokinetics, safety and antitumor activity obtained from both phase IA and IB determined the tislelizumab recommended dose; ultimately, tislelizumab 200 mg intravenous every 3 weeks was the dose and schedule recommended to be taken into subsequent clinical trials. Conclusions Tislelizumab monotherapy demonstrated an acceptable safety/tolerability profile. Durable responses were observed in heavily pretreated patients with advanced solid tumors, supporting the evaluation of tislelizumab 200 mg every 3 weeks, as monotherapy and in combination therapy, for the treatment of solid tumors and hematological malignancies. Trial registration number NCT02407990.Copyright © Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.en
dc.languageEnglishen
dc.languageenen
dc.publisherBMJ Publishing Group (E-mail: subscriptions@bmjgroup.com)en
dc.relation.ispartofJournal for ImmunoTherapy of Canceren
dc.subject.meshhypercalcemia-
dc.subject.meshhyperglycemia-
dc.subject.meshhypertransaminasemia-
dc.subject.meshhypokalemia-
dc.subject.meshhyponatremia-
dc.subject.meshliver cell carcinoma-
dc.subject.meshloss of appetite-
dc.subject.meshlower respiratory tract infection-
dc.subject.meshlung embolism-
dc.subject.meshmaximum tolerated dose-
dc.subject.meshmelanoma-
dc.subject.meshmerkel cell carcinoma-
dc.subject.meshmicrosatellite instability-
dc.subject.meshmonotherapy-
dc.subject.meshmultiple cycle treatment-
dc.subject.meshnausea and vomiting-
dc.subject.meshnon small cell lung cancer-
dc.subject.meshoptimal drug dose-
dc.subject.meshovary carcinoma-
dc.subject.meshpancreas cancer-
dc.subject.meshphase 1-
dc.subject.meshpleura effusion-
dc.subject.meshpneumonia-
dc.subject.meshrash-
dc.subject.meshrecommended drug dose-
dc.subject.meshrenal cell carcinoma-
dc.subject.meshsepsis-
dc.subject.meshskin carcinoma-
dc.subject.meshsmall intestine obstruction-
dc.subject.meshsolid malignant neoplasm-
dc.subject.meshstomach cancer-
dc.subject.meshtime to maximum plasma concentration-
dc.subject.meshtriple negative breast cancer-
dc.subject.meshupper gastrointestinal-
dc.subject.meshbilirubin-
dc.subject.meshnew drug/ct-
dc.subject.meshnew drug-
dc.subject.meshprogrammed 1 ligand 1-
dc.subject.meshtislelizumab [Adverse Drug Reaction]-
dc.subject.meshtislelizumab/ct-
dc.subject.meshtislelizumab-
dc.subject.meshimmunohistochemical test kit-
dc.subject.meshVENTANA PD-L1 (SP263)-
dc.subject.meshmaximum concentration-
dc.subject.meshaged-
dc.subject.meshanemia-
dc.subject.meshantineoplastic activity-
dc.subject.meshascites-
dc.subject.meshbackache-
dc.subject.meshbile duct carcinoma-
dc.subject.meshbody weight disorder-
dc.subject.meshcolitis-
dc.subject.meshcolorectal cancer-
dc.subject.meshconstipation-
dc.subject.meshcoughing-
dc.subject.meshdiarrhea-
dc.subject.meshdrug dosage form comparison-
dc.subject.meshdrug dose escalation-
dc.subject.meshdrug dose regimen-
dc.subject.meshdrug efficacy-
dc.subject.meshdrug half life-
dc.subject.meshdrug safety-
dc.subject.meshdrug tolerability-
dc.subject.meshdrug withdrawal-
dc.subject.meshdysphagia-
dc.subject.meshdyspnea-
dc.subject.meshesophagus cancer-
dc.subject.meshesophagus carcinoma-
dc.subject.meshfatigue-
dc.subject.meshgastrointestinal stromal tumor-
dc.subject.meshhead and neck squamous cell carcinoma-
dc.subject.meshhyperbilirubinemia-
dc.titlePhase IA/IB study of single-agent tislelizumab, an investigational anti-PD-1 antibody, in solid tumors.en
dc.typeArticleen
dc.type.studyortrialObservational study (cohort, case-control, cross sectional or survey)-
dc.identifier.doihttp://monash.idm.oclc.org/login?url=http://dx.doi.org/10.1136/jitc-2019-000453-
dc.publisher.placeUnited Kingdomen
dc.identifier.pubmedid32540858 [http://www.ncbi.nlm.nih.gov/pubmed/?term=32540858]en
dc.identifier.source632075310en
dc.identifier.institution(Desai, Sandhu) Peter MacCallum Cancer Centre, University of Melbourne, Melbourne, VIC, Australia (Deva, Barlow) Auckland City Hospital, Auckland, New Zealand (Lee) Seoul National University Bundang Hospital, Seongnam-si, South Korea (Lin) National Taiwan University Hospital, Taipei, Taiwan (Republic of China) (Yen) National Cheng Kung University Hospital, Tainan, Taiwan (Republic of China) (Chao) Taipei Veterans General Hospital, Taipei, Taiwan (Republic of China) (Keam, Lee) Seoul National University Hospital, Seoul, South Korea (Jameson) Waikato Hospital, University of Auckland Waikato Clinical Campus, Hamilton, New Zealand (Hou) Chang Gung Memorial Hospital, Chang Gung University, Linkou, Taiwan (Republic of China) (Kang) Asan Medical Center, Seoul, South Korea (Markman) Monash Health, Monash University, Clayton, VIC, Australia (Lu) Chang Gung Memorial Hospital, Chia-yi, Taiwan (Republic of China) (Rau) Division of Pulmonary and Critical Care Medicine, Department of Internal Medicine, Kaohsiung Chang Gung Memorial Hospital, Kaohsiung, Taiwan (Republic of China) (Horvath) Chris o'Brien Lifehouse, Sydney, NSW, Australia (Horvath) Sydney Medical School, University of Sydney, Sydney, NSW, Australia (Friedlander) Department of Medical Oncology, Prince of Wales Hospital and Prince of Wales Clinical School, University of New South Wales, Sydney, NSW, Australia (Hill) Tasman Oncology Research Ltd, Southport, QLD, Australia (Wu, Wu, Paton) BeiGene USA, Inc, San Mateo, California, United States (Zhang, Liang) BeiGene (Beijing) Co., Ltd, Beijing, China (Millward) Linear Clinical Research, Nedlands, WA, Australiaen
dc.description.addressJ. Desai, 3Division of Pulmonary and Critical Care Medicine, Department of Internal Medicine, Kaohsiung Chang Gung Memorial Hospital, Kaohsiung, Taiwan (Republic of China). E-mail: Jayesh.Desai@petermac.orgen
dc.description.publicationstatusEmbaseen
dc.rights.statementCopyright 2020 Elsevier B.V., All rights reserved.en
dc.subect.keywordsimmunotherapy oncology programmed cell death 1 receptor tumorsen
dc.identifier.authoremailDesai J.; Jayesh.Desai@petermac.orgen
item.fulltextNo Fulltext-
item.cerifentitytypePublications-
item.openairetypeArticle-
item.openairecristypehttp://purl.org/coar/resource_type/c_18cf-
item.grantfulltextnone-
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