Abstract CT027: A phase I, open-label study of GSK3174998 administered alone and in combination with pembrolizumab in patients (pts) with selected advanced solid tumors (ENGAGE-1)

Infante, Jeffrey R.; Ahlers, Christoph M.; Hodi, F. Stephen; Postel-Vinay, S.; Schellens, Jan H.M.; Heymach, John V.; Autio, Karen A.; Barnette, Mary S.; Struemper, Herbert; Watmuff, Maura; Paul, Elaine; Kaufman, David R.; Weber, Jeffrey S.; Hoos, Axel

doi:10.1158/1538-7445.am2016-ct027

Cited by 3 publications

(7 citation statements)

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“…In accordance with disappointing clinical trial results, [27][28][29] the clinical candidate human αOX40 IgG2 antibody failed to stimulate TIL proliferation or cytokine secretion in our in vitro expansion assay, while treatment with OX40L resulted in TIL expansion and increased secretion of proinflammatory cytokines. The clinical αOX40 antibody and OX40L differ with regard to their structure: αOX40 antibody is monomeric, whereas OX40L is of hexameric shape.…”

Section: Discussionsupporting

confidence: 81%

“…27 Besides, more phase I studies have been performed in which agonistic αOX40 antibody treatment showed low clinical efficacy in advanced solid tumors. 28 29 Hence, we wondered whether the reason for the limited clinical efficacy was due to (1) low OX40 expression on human TILs, (2) minor effects of OX40 costimulation on TIL functions and expansion, or (3) suboptimal performance of the currently used αOX40 antibodies. Therefore, we measured OX40 levels on distinct TIL subsets of colorectal and HCC tumor tissue, thus demonstrating that TI activated T-helper (aTh) and activated regulatory T cell (aTreg) do express high OX40 levels.…”

Section: Introductionmentioning

confidence: 99%

“…27 Besides, more phase I studies have been performed in which agonistic αOX40 antibody treatment showed low clinical efficacy in advanced solid tumors. 28 29 …”

Section: Introductionmentioning

confidence: 99%

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FcγRIIB engagement drives agonistic activity of Fc-engineered αOX40 antibody to stimulate human tumor-infiltrating T cells

Carrascosa

Beek

Ruiter

et al. 2020

J Immunother Cancer

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BackgroundOX40 (CD134) is a costimulatory molecule of the tumor necrosis factor receptor superfamily that is currently being investigated as a target for cancer immunotherapy. However, despite promising results in murine tumor models, the clinical efficacy of agonistic αOX40 antibodies in the treatment of patients with cancer has fallen short of the high expectation in earlier-stage trials.MethodsUsing lymphocytes from resected tumor, tumor-free (TF) tissue and peripheral blood mononuclear cells (PBMC) of 96 patients with hepatocellular and colorectal cancers, we determined OX40 expression and the in vitro T-cell agonistic activity of OX40-targeting compounds. RNA-Seq was used to evaluate OX40-mediated transcriptional changes in CD4+ and CD8+ human tumor-infiltrating lymphocytes (TILs).ResultsHere, we show that OX40 was overexpressed on tumor-infiltrating CD4+ T cells compared with blood and TF tissue-derived T cells. In contrast to a clinical candidate αOX40 antibody, treatment with an Fc-engineered αOX40 antibody (αOX40_v12) with selectively enhanced FcγRIIB affinity, stimulated in vitro CD4+ and CD8+ TIL expansion, as well as cytokine and chemokine secretions. The activity of αOX40_v12 was dependent on FcγRIIB engagement and intrinsic CD3/CD28 signals. The transcriptional landscape of CD4+ and CD8+ TILs shifted toward a prosurvival, inflammatory and chemotactic profile on treatment with αOX40_v12.ConclusionsOX40 is overexpressed on CD4+ TILs and thus represents a promising target for immunotherapy. Targeting OX40 with currently used agonistic antibodies may be inefficient due to lack of OX40 multimerization. Thus, Fc engineering is a powerful tool in enhancing the agonistic activity of αOX40 antibody and may shape the future design of antibody-mediated αOX40 immunotherapy.

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Section: Discussionsupporting

confidence: 81%

Section: Introductionmentioning

confidence: 99%

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FcγRIIB engagement drives agonistic activity of Fc-engineered αOX40 antibody to stimulate human tumor-infiltrating T cells

Carrascosa

Beek

Ruiter

et al. 2020

J Immunother Cancer

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“…Он трансдуцирует костимулирующий сигнал во время активации Т-клеток. Пациенты с мРМП активно включаются в несколько исследований фазы I, в которых изучаются антагонисты TIM-3 (NCT02608268) [42], ингибиторы LAG3 (NCT01968109) [43] и агонисты OX40 (NCT02528357) [44], с ингибиторами PD-1/PD-L1 и без них. В настоящее время анти-LAG3 mAb (BMS-986016) изучается в сочетании с ниволумабом в исследовании I фазы (NCT01968109) [43].…”

Section: комбинации ингибиторов иммунных контрольных точекunclassified

“…В настоящее время анти-LAG3 mAb (BMS-986016) изучается в сочетании с ниволумабом в исследовании I фазы (NCT01968109) [43]. Агонист OX40 (GSK3174998) исследуется совместно с пембролизумабом в испытании фазы I (NCT02528357) [44]. Еще один интересный подход к стимулированию иммунного ответа дополнительно нацелен на Т-клеточное микроокружение и связан с индоламин-2,3-диоксигеназой, которая является внутриклеточным ферментом, вырабатываемым опухолевыми клетками, и играет важную роль в путях, генерирующих иммуносупрессивные метаболиты [45].…”

Section: комбинации ингибиторов иммунных контрольных точекunclassified

Immune checkpoint inhibitors for bladder cancer treatment

Солодкий¹,

Radiology²,

Pavlov³

et al. 2020

Russian Medical Review

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Уротелиальный рак (переходноклеточный рак) является наиболее распространенным гистологическим типом злокачественных новообразований верхних и нижних мочевых путей. В настоящее время химиотерапия на основе платины является стандартным методом лечения метастатического рака мочевого пузыря (РМП) и предпочтительным вариантом лечения в периоперационном (неоадъювантном и/или адъювантном) периоде при мышечно-инвазивном раке мочевого пузыря. Кроме того, применяется внутрипузырная иммунотерапия (БЦЖ-вакцина) в качестве адъювантного терапевтического варианта при мышечно-неинвазивном раке мочевого пузыря после трансуретральной резекции для предотвращения рецидива и прогрессирования заболевания. В последние годы все чаще стала применяться системная иммунотерапия, направленная на ингибирование иммунных контрольных точек. Запрограммированный рецептор клеточной гибели 1 (PD-1) и его лиганд (PD-L1) являются важными негативными регуляторами иммунной активности, предотвращающими разрушение нормальных тканей и развитие аутоммунных реакций. На сегодняшний день 5 ингибиторов иммунных контрольных точек, блокирующих PD-1 (пембролизумаб, ниволумаб) или PD-L1 (атезолизумаб, дурвалумаб и авелумаб), одобрены Управлением по контролю качества пищевых продуктов и медикаментов США для использования в 1-й и 2-й линии лечения метастатического РМП (мРМП). В обзоре рассмотрены данные клинических исследований ингибиторов иммунных контрольных точек в лечении локализованного РМП и мРМП.

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Immune checkpoint inhibitors for urothelial carcinoma

Kim

Seo

2018

Investig Clin Urol

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Urothelial carcinoma (UC), originating in the bladder or upper urinary tract, is the most common histological type of cancer. Currently, platinum-based cytotoxic chemotherapy is the standard treatment for metastatic UC (mUC) and the preferred treatment option in the perioperative (neoadjuvant and/or adjuvant) setting of muscle invasive bladder cancer (MIBC). In addition, intravesical bacillus Calmette-Guerin immunotherapy or chemotherapy is applied as the adjuvant therapeutic option in non-muscle invasive bladder cancer (NMIBC) after transurethral resection, to prevent recurrence and progression. In recent years, with an increased understanding of cancer immunobiology, systemic immunotherapies targeting immune checkpoint inhibition has been explored and clinically used in the area of UC. The programmed cell death 1 receptor (PD-1) and its ligand (PD-L1) are important negative regulators of immune activity, preventing the destruction of normal tissues and autoimmunity. To date, five immune checkpoint inhibitors blocking PD-1 (pembrolizumab, nivolumab) or PD-L1 (atezolizumab, durvalumab, and avelumab) have been approved by the United States Food and Drug Administration (US-FDA) for first- or second-line use in mUC, based on durable therapeutic response and manageable safety profiles observed in relevant clinical trials. In addition, the clinical use of several immune checkpoint inhibitors is currently being tested for MIBC and NMIBC. In this article, we review the current and ongoing clinical trials, regarding immune checkpoint inhibitors, being conducted in various clinical settings of UC, including mUC, MIBC, and NMIBC.

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Abstract CT027: A phase I, open-label study of GSK3174998 administered alone and in combination with pembrolizumab in patients (pts) with selected advanced solid tumors (ENGAGE-1)

Cited by 3 publications

References 0 publications

FcγRIIB engagement drives agonistic activity of Fc-engineered αOX40 antibody to stimulate human tumor-infiltrating T cells

FcγRIIB engagement drives agonistic activity of Fc-engineered αOX40 antibody to stimulate human tumor-infiltrating T cells

Immune checkpoint inhibitors for bladder cancer treatment

Immune checkpoint inhibitors for urothelial carcinoma

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