Your search keyword '"nausea"' showing total 377 results

1. A first-in-human phase I trial of daily oral zelenirstat, a N-myristoyltransferase inhibitor, in patients with advanced solid tumors and relapsed/refractory B-cell lymphomas.

Author

Sangha, Randeep, Jamal, Rahima, Spratlin, Jennifer, Kuruvilla, John, Sehn, Laurie H., Beauchamp, Erwan, Weickert, Michael, Berthiaume, Luc G., and Mackey, John R.

Subjects

BREAST cancer prognosis, MELANOMA prognosis, DRUG toxicity, FEBRILE neutropenia, DIARRHEA, GASTROINTESTINAL tumors, APPENDIX (Anatomy), PHYSICAL diagnosis, PATIENT compliance, ADENOCARCINOMA, GALLBLADDER tumors, BLADDER tumors, SQUAMOUS cell carcinoma, ANEMIA, CANCER relapse, RESEARCH funding, LIQUID chromatography-mass spectrometry, MELANOMA, ANTINEOPLASTIC agents, INVESTIGATIONAL drugs, CLINICAL trials, FATIGUE (Physiology), OVARIAN tumors, COMPUTED tomography, BLOOD collection, ABDOMINAL pain, BREAST tumors, LEIOMYOSARCOMA, CHOLANGITIS, ORAL drug administration, CANCER patients, COLORECTAL cancer, POSITRON emission tomography computed tomography, DESCRIPTIVE statistics, PROSTATE tumors, PLEURAL tumors, FEVER, SMALL molecules, EXPERIMENTAL design, THROMBOCYTOPENIA, KAPLAN-Meier estimator, PANCREATIC tumors, DRUG efficacy, RESEARCH, BLOOD plasma, ANOREXIA nervosa, LUNG tumors, GASTRITIS, VOMITING, PROGRESSION-free survival, DRUGS, ANAL tumors, MESOTHELIOMA, DIVERTICULITIS, B cell lymphoma, DRUG tolerance, HEMORRHAGE, NEUTROPENIA, NAUSEA, OVERALL survival, DISEASE progression, GASTROESOPHAGEAL reflux, DEHYDRATION, HYPOPHOSPHATEMIA

Abstract

Myristoylation, the N-terminal addition of the fatty acid myristate to proteins, regulates membrane-bound signal transduction pathways important in cancer cell biology. This modification is catalyzed by two N-myristoyltransferases, NMT1 and NMT2. Zelenirstat is a first-in-class potent oral small molecule inhibitor of both NMT1 and NMT2 proteins. Patients with advanced solid tumors and relapsed/refractory (R/R) B-cell lymphomas were enrolled in an open label, phase I dose escalation trial of oral daily zelenirstat, administered in 28-day cycles until progression or unacceptable toxicity. The endpoints were to evaluate dose-limiting toxicities (DLT) to establish a maximum tolerated dose (MTD), pharmacokinetic parameters, and anticancer activity. Twenty-nine patients were enrolled (25 advanced solid tumor; 4 R/R B-cell lymphoma) and 24 were DLT-evaluable. Dosing ranged from 20 mg once daily (OD) to 210 mg OD without DLT, but gastrointestinal DLTS were seen in the 280 mg cohort. MTD and recommended phase 2 dose were 210 mg OD. Common adverse events were predominantly Gr ≤ 2 nausea, vomiting, diarrhea, and fatigue. Plasma concentrations peaked at 2 h with terminal half-lives averaging 10 h. Steady state was achieved by day 15, and higher doses achieved trough concentrations predicted to be therapeutic. Stable disease as best response was seen in eight (28%) patients. Progression-free survival and overall survival were significantly better in patients receiving 210 mg OD compared to those receiving lower doses. Zelenirstat is well-tolerated, achieves plasma exposures expected for efficacy, and shows early signs of anticancer activity. Further clinical development of zelenirstat is warranted. [ABSTRACT FROM AUTHOR]

Published

2024

2. Liposomal irinotecan (HR070803) in combination with 5-fluorouracil and leucovorin in patients with advanced solid tumors: a phase 1b dose-escalation and expansion study.

Author

Ji, Dongmei, Shen, Weina, Li, Ting, Wang, Huan, Bai, Jianling, Cao, Junning, and Hu, Xichun

Subjects

THERAPEUTIC use of antineoplastic agents, IRINOTECAN, COMBINATION drug therapy, DRUG toxicity, FEBRILE neutropenia, LEUCOPENIA, DIARRHEA, PATIENT safety, RESEARCH funding, CLINICAL trials, FATIGUE (Physiology), CANCER patients, DRUG dosage, DOSE-effect relationship in pharmacology, INTRAVENOUS therapy, FOLINIC acid, DRUG efficacy, ANOREXIA nervosa, FLUOROURACIL, TUMORS, DRUG tolerance, NEUTROPENIA, NAUSEA, EVALUATION

Abstract

This phase 1b study aimed to evaluate the dose-limiting toxicity (DLT), maximum tolerated dose (MTD), pharmacokinetics, and preliminary efficacy of HR070803, a novel nanoliposomal formulation of irinotecan, in combination with 5-fluorouracil and leucovorin in patients with pretreated advanced solid tumors. This study consisted of dose-escalation and expansion stages. Dose escalation was performed with a traditional 3 + 3 design; patients received intravenous infusion of HR070803 from 60 to 80 mg/m2, followed by leucovorin (200 mg/m2) and 5-fluorouracil (2000 mg/m2) every 2 weeks. In the expansion stage, patients received treatments at selected tolerable dose. Fifteen patients received treatments at 60 mg/m2 (n = 12) and 80 mg/m2 (n = 3). DLTs occurred in 2 patients at 80 mg/m2 (grade 2 neutropenia that resulted in a dose delay of ≥ 7 days, n = 1; grade 3 febrile neutropenia, n = 1). The MTD was determined to be 60 mg/m2. The most frequent HR070803related adverse events included anorexia, leukopenia, neutropenia, nausea, fatigue, and diarrhea. SN-38, the active metabolite of irinotecan, exhibited lower maximum plasma concentrations and a prolonged terminal half-life when irinotecan was administered via nanoliposome compared to conventional injection. Overall, 4 patients achieved a partial response (confirmed, n = 2), and 9 had stable disease. The MTD of HR070803 was 60 mg/m2 when infused with 5-fluorouracil and leucovorin. Nanoliposomal encapsulation modified the pharmacokinetics of irinotecan and SN-38. HR070803 with 5-fluorouracil and leucovorin demonstrated a manageable safety profile and promising antitumor efficacy in advanced solid tumors. Trial registration: Clinicaltrials.gov, NCT05086848. Retrospectively registered on Oct. 12, 2021. [ABSTRACT FROM AUTHOR]

Published

2024

3. A phase 1b open-label study to evaluate the safety, tolerability, pharmacokinetics, and pharmacodynamics of py314 in combination with pembrolizumab in patients with advanced renal cell carcinoma.

Author

Beckermann, Kathryn E., Patnaik, Amita, Winer, Ira, Tan, Winston, Bashir, Babar, Kyriakopoulos, Christos E., Sweis, Randy F., Chamberlain, Marc, and Rini, Brian I.

Subjects

THERAPEUTIC use of antineoplastic agents, THERAPEUTIC use of monoclonal antibodies, PATIENT safety, MACROPHAGES, RESEARCH funding, CLINICAL trials, IMMUNOTHERAPY, FATIGUE (Physiology), ANTINEOPLASTIC agents, DESCRIPTIVE statistics, FEVER, METASTASIS, MONOCLONAL antibodies, GENE expression, RENAL cell carcinoma, COMPARATIVE studies, DRUG tolerance, IMMUNOSUPPRESSION, NAUSEA

Abstract

Summary: Checkpoint inhibition (CPI) is a standard therapeutic approach in metastatic renal cell carcinoma (RCC). However, not all patients respond to CPI, and the immune suppressive characteristics of the RCC tumor microenvironment may contribute to treatment failure. Triggering Receptor Expressed on Myeloid Cells-2 (TREM2) is a transmembrane protein expressed on a subset of myeloid cells with M2-like anti-inflammatory properties that has previously been associated with disease recurrence after nephrectomy and poor outcomes when expressed at high levels. PY314 is a humanized monoclonal antibody targeting TREM2 that depletes tumor-associated macrophages. In this study, the combination of PY314 and pembrolizumab was investigated in patients with CPI-refractory RCC. Eligible patients had clear cell RCC with disease progression on prior CPI either in combination or sequentially with VEGF-TKI. Patients were treated with PY314 10 mg/kg in combination with pembrolizumab 200 mg IV every 21 days. The primary objective was to assess safety and tolerability and secondary objectives included pharmacokinetics and anti-tumor activity by RECIST v1.1. Seventeen patients were enrolled with a median age of 67 years, 82% male, 100% had prior CPI, and 76% had received three or more prior lines of therapy. The combination of PY314 and pembrolizumab demonstrated an acceptable safety profile with 47.1% any grade treatment-related adverse events (AE) (including only 5.9% grade ≥ 3), the most common being fatigue, pyrexia, nausea, and infusion-related reactions. One patient achieved a partial response (6%), and four patients had stable disease (24%) as their best response. The median PFS was 1.4 months (95% CI 1.2- 3.8). The combination of PY314 and pembrolizumab was safe, but the limited anti-tumor effect observed suggests that TREM2 targeting in conjunction with PD-1 blockade may not overcome resistance to prior CPI. Further investigation is warranted to determine if improved efficacy can be achieved in IO-naïve settings. Trial Registration: NCT04691375 [ABSTRACT FROM AUTHOR]

Published

2024

4. A multicenter phase II trial of the triplet antiemetic therapy with palonosetron, aprepitant, and olanzapine for a cisplatin-containing regimen. - PATROL-I-.

Author

Tsuji, Daiki, Nakagaki, Shigeru, Yonezawa, Itsuki, Suzuki, Kenichi, Yokokawa, Takashi, Kawasaki, Yohei, Yamaguchi, Takumi, Kawaguchi, Takashi, Hatori, Masahiro, Matsumoto, Takuma, Sakata, Yukio, Yamamoto, Keisuke, Nishimura, Tomoyasu, Kogure, Yuki, Hayashi, Toshinobu, Osawa, Misa, Itoh, Kunihiko, and Watanabe, Masaya

Subjects

DRUG efficacy, NAUSEA, CLINICAL trials, CONFIDENCE intervals, CANCER chemotherapy, DEXAMETHASONE, HEALTH outcome assessment, VOMITING, CISPLATIN, KAPLAN-Meier estimator, RESEARCH funding, DESCRIPTIVE statistics, ANOREXIA nervosa, ANTIEMETICS, PATIENT safety, PHARMACODYNAMICS

Abstract

Summary: Dexamethasone is one of the key antiemetic agents and is widely used even now. However, dexamethasone has been associated with several adverse reactions even after short-term administration. Therefore, developing a steroid-free antiemetic regimen is an important issue to consider. Thus, the purpose of this study was to investigate the efficacy and safety of palonosetron, aprepitant, and olanzapine in a multi-institutional phase II study. Chemotherapy-naive patients scheduled to receive cisplatin were enrolled and evaluated for the occurrence of chemotherapy-induced nausea and vomiting during 120 h after chemotherapy. The primary endpoint of the study was total control (TC) in the overall phase. The key secondary endpoint was complete response (CR), which was assessed in the acute, delayed, and overall phase, respectively. Adverse events were evaluated according to the Common Terminology Criteria for Adverse Events. Eighty-five patients were enrolled from 8 centers in Japan, of which 83 were evaluable for analyses. The percentage of patients who achieved TC during the overall phase was 31.3%. CR was achieved in 61.4%, 84.3%, and 65.1% of patients during the overall, acute, and delayed phases, respectively. The most frequently reported adverse event was anorexia. The primary endpoint was below the threshold and we could not find benefit in the dexamethasone-free regimen, but CR during the overall phase was similar to that of the conventional three-drug regimen. This antiemetic regimen without dexamethasone might be an option for patients for whom corticosteroids should not be an active application. [ABSTRACT FROM AUTHOR]

Published

2024

5. Lurbinectedin in patients with pretreated endometrial cancer: results from a phase 2 basket clinical trial and exploratory translational study.

Author

Kristeleit, Rebecca, Leary, Alexandra, Delord, Jean Pierre, Moreno, Victor, Oaknin, Ana, Castellano, Daniel, Shappiro, Geoffrey I., Fernández, Cristian, Kahatt, Carmen, Alfaro, Vicente, Siguero, Mariano, Rueda, Daniel, Zeaiter, Ali, Awada, Ahmad, Santaballa, Ana, Zaman, Khalil, Sehouli, Jalid, and Subbiah, Vivek

Subjects

RESEARCH, APPETITE, INTRAVENOUS therapy, CLINICAL trials, CONFIDENCE intervals, NAUSEA, FEBRILE neutropenia, TIME, CONSTIPATION, ANTINEOPLASTIC agents, NEUTROPENIA, TREATMENT effectiveness, VOMITING, ENDOMETRIAL tumors, RESEARCH funding, TRANSLATIONAL research, PROGRESSION-free survival, ODDS ratio, DRUG side effects, FATIGUE (Physiology), OVERALL survival, PATIENT safety, DRUG toxicity

Abstract

Second-line treatment of endometrial cancer is an unmet medical need. Lurbinectedin showed promising antitumor activity in a phase I study in combination with doxorubicin in advanced endometrial cancer. This phase 2 Basket trial evaluated lurbinectedin 3.2 mg/m2 1-h intravenous infusion every 3 weeks in a cohort of 73 patients with pretreated endometrial cancer. The primary endpoint was overall response rate (ORR) according to RECIST v1.1. Secondary endpoints included duration of response (DoR), progression-free survival (PFS), overall survival (OS), safety and an exploratory translational study. Confirmed complete (CR) and partial response (PR) was reported in two and six patients, respectively (ORR = 11.3%; 95%CI, 5.0–21.0%). Median DoR was 9.2 months (95%CI, 3.4–18.0 months), median PFS was 2.6 months (95%CI, 1.4–4.0 months) and median OS was 9.3 months (95%CI, 6.1–12.8 months). Molecular subtypes showed differences in PFS rate at 6 months (p53abn 23.7% vs. "No Specific Molecular Profile" [NSMP] 42.9%) and median OS (p53abn 6.6 months vs. NSMP 16.1 months). The most common treatment-related adverse events (mostly grade 1/2) were fatigue (54.8% of patients), nausea (50.7%), vomiting (26.0%) decreased appetite (17.8%). and constipation, (19.2%). The most common grade 3/4 toxicity was neutropenia (43.8%; grade 4, 19.2%; febrile neutropenia, 4.1%). In conclusion, considering the exploratory aim of this trial and the hints of antitumor activity observed together with a predictable and manageable safety profile, further biomarker-based development of lurbinectedin is recommended in this indication in combination with other agents. Clinicaltrials.gov identifier: NCT02454972. [ABSTRACT FROM AUTHOR]

Published

2023

6. A phase 1 study to assess the safety, pharmacokinetics, and anti-tumor activity of the androgen receptor n-terminal domain inhibitor epi-506 in patients with metastatic castration-resistant prostate cancer.

Author

Maurice-Dror, Corinne, Le Moigne, Ronan, Vaishampayan, Ulka, Montgomery, Robert B., Gordon, Michael S., Hong, Nan Hyung, DiMascio, Leah, Perabo, Frank, and Chi, Kim N.

Subjects

CLINICAL trials, DRUG dosage, DIARRHEA, NAUSEA, ANTINEOPLASTIC agents, METASTASIS, CANCER patients, AMYLASES, ANDROGEN receptors, ABDOMINAL pain, PROSTATE-specific antigen, FATIGUE (Physiology), DRUG toxicity

Abstract

Summary: Background. EPI-506 is the first of a new class of drugs targeting the N-terminal domain (NTD) of the androgen receptor (AR), potentially overcoming known resistance mechanisms to androgen receptor pathway inhibitors (ARPIs) among men with metastatic castration resistant prostate cancer (mCRPC). Methods. Patients with mCRPC who had progressed on prior ARPI were enrolled in this phase 1 open-label, adaptive 3 + 3 dose escalation study. The primary outcome was safety and tolerability of oral EPI-506. Secondary objectives included determination of the maximal tolerated dose (MTD), pharmacokinetic profile, and antitumor efficacy. Results. 28 mCRPC patients were enrolled into 7 dose cohorts of EPI-506 ranging from 80-3600 mg given once daily and 1800 mg given twice daily. Six DLTs occurred in 4 patients; Grade 4 elevated amylase; Grade 3 abdominal pain; Grade 3 elevated ALT and Grade 3 elevated AST; Grade 2 nausea and Grade 1 vomiting which resulted in study drug intake of < 75% of the expected dose during the DLT assessment period. The most common drug-related adverse events included diarrhea, nausea and fatigue. Six patients had a PSA decline not meeting PSA response criteria. The study was terminated prior to reaching the MTD due to poor oral bioavailability. Conclusions. This phase 1 trial established the safety of EPI-506 and provides proof of concept for targeting the AR NTD. Next generation compounds with improved bioavailability and potency are in clinical development. [ABSTRACT FROM AUTHOR]

Published

2022

7. A phase I trial of lurbinectedin in combination with cisplatin in patients with advanced solid tumors.

Author

Metaxas, Yannis, Kahatt, Carmen, Alfaro, Vicente, Fudio, Salvador, Zeaiter, Ali, Plummer, Ruth, Sessa, Cristiana, Von Moos, Roger, Forster, Martin, and Stathis, Anastasios

Subjects

CLINICAL trials, INTRAVENOUS therapy, LEUCOPENIA, NAUSEA, ORAL drug administration, ANTINEOPLASTIC agents, NEUTROPENIA, CANCER patients, LYMPHOPENIA, ALKYLATING agents, CISPLATIN, BLOOD diseases, CANCER fatigue, TUMORS, DRUG side effects, ANTIEMETICS, DRUG toxicity

Abstract

Summary: Background In vitro/in vivo data showed synergism of cisplatin and lurbinectedin in ovarian cancer cells and grafts. This phase I trial investigated the recommended phase II dose (RD) of cisplatin and lurbinectedin combination, with (Group A) or without aprepitant (Group B), in patients with advanced solid tumors. Patients and Methods All patients received 60 mg/m2 cisplatin 90-min intravenous (i.v.) infusion followed by lurbinectedin 60-min i.v. infusion at escalating doses on Day 1 every 3 weeks (q3wk). Patients in Group A additionally received orally 125 mg aprepitant one hour before cisplatin on Day 1 and 80 mg on Days 2 and 3. Toxicity was graded according to the NCI-CTCAE v.4. Results RD for Group A was cisplatin 60 mg/m2 plus lurbinectedin 1.1 mg/m2. RD for Group B was cisplatin 60 mg/m2 plus lurbinectedin 1.4 mg/m2. The most frequent grade ≥ 3 adverse events were hematological [neutropenia (41%), lymphopenia (35%), leukopenia (24%), thrombocytopenia (18%)] and fatigue (35%) in Group A (n = 17), and neutropenia (50%), leukopenia (42%), lymphopenia (29%), and fatigue (13%) and nausea (8%) in Group B (n = 24). Four patients (2 in each group) had a partial response. Disease stabilization for ≥ 4 months was observed in 4 and 10 patients, respectively. Conclusion The combination of lurbinectedin with cisplatin was not possible in meaningful therapeutic dosage due to toxicity. The addition of aprepitant in combination with cisplatin did not allow increasing the dose due to hematological toxicity, whereas omitting aprepitant increased the incidence of nausea and vomiting. Modest clinical activity was observed in general. Clinical trial registrationwww.ClinicalTrials.gov code: NCT01980667. Date of registration: 11 November 2013. [ABSTRACT FROM AUTHOR]

Published

2022

8. A multicenter phase 1/2 study investigating the safety, pharmacokinetics, pharmacodynamics and efficacy of a small molecule antimetabolite, RX-3117, plus nab-paclitaxel in pancreatic adenocarcinoma.

Author

Babiker, Hani, Schlegel, Peter J., Hicks, Lee G., Bullock, Andrea J., Burhani, Nafisa, Mahadevan, Daruka, Elquza, Emad, Borad, Mitesh J., Benaim, Ely, Peterson, Christine, Heaton, Callie, and Ocean, Allyson J.

Subjects

PANCREATIC tumors, ADENOCARCINOMA, SAFETY, DRUG efficacy, RESEARCH, CLINICAL trials, DRUG tolerance, INTRAVENOUS therapy, DIARRHEA, NAUSEA, METASTASIS, ANTINEOPLASTIC agents, MEDICAL cooperation, TREATMENT duration, ANTIMETABOLITES, TREATMENT effectiveness, COMPARATIVE studies, KAPLAN-Meier estimator, SURVIVAL analysis (Biometry), DESCRIPTIVE statistics, PACLITAXEL, ETHNIC groups, DRUG side effects, FATIGUE (Physiology), DATA analysis software, PHARMACODYNAMICS

Abstract

Summary: Background RX-3117 is an oral small molecule antimetabolite, cyclopentyl pyrimidyl nucleoside that is activated by cancer cells over-expressing uridine cytidine kinase 2 (UCK2). Single agent RX-3117 demonstrated efficacy in a phase I trial in patients with metastatic (met) pancreatic adenocarcinoma (PC). RX-3117 plus nab-paclitaxel (nab-Pac) was evaluated as a first line treatment in met-PC cancer. Methods This was a multicenter open label phase I/II 2-stage study investigating the combination of RX3117 plus nab-Pac in the frontline treatment of patients with met-PC. The phase I portion comprised a dose de-escalation design with primary objectives of determining the safety, tolerability and recommended phase 2 dose (RP2D) of RX-3117 (orally 700, 600, or 500 mg/day for 5 consecutive days with 2 days off/week) plus nab-Pac (intravenous (IV) 125 mg/m2 once weekly) for 3 weeks with 1 week off per a 4-week cycle. The primary objective was to determine the antitumor efficacy. Results 46 patients were enrolled (22 male/24 female; median age 67; 91% Caucasian). The RP2D of RX-3117 plus nab-Pac was 700 mg/day. No dose-limiting toxicities were observed (DLTs). The overall response rate (ORR) was 23.1% and disease control rate (DCR) 74.4%. RX-3117 pharmacokinetics (PK) results were similar to previously reported monotherapy phase 1 trial. All patients experienced a treatment emergent adverse event (TEAE) with the most common diarrhea, nausea, and fatigue.10.9% of patients experienced a serious adverse event (SAE) related to the combination. Conclusion RX-3117 plus nab-Pac in newly diagnosed met-PC patients demonstrated tolerability, safety, and early treatment efficacy. [ABSTRACT FROM AUTHOR]

Published

2022

9. Selinexor in combination with topotecan in patients with advanced or metastatic solid tumors: Results of an open-label, single-center, multi‐arm phase Ib study.

Author

Thein, Kyaw Zin, Piha-Paul, Sarina A., Tsimberidou, Apostolia, Karp, Daniel D., Janku, Filip, Zarifa, Abdulrazzak, Shah, Jatin, Milton, Denái R., Bean, Stacie, McQuinn, Lacey, Gong, Jing, Colen, Rivka, Carter, Brett W., Subbiah, Vivek, Ogbonna, Deby C., Pant, Shubham, Meric-Bernstam, Funda, and Naing, Aung

Subjects

THERAPEUTIC use of antineoplastic agents, DRUG efficacy, TOPOTECAN, CLINICAL trials, NAUSEA, METASTASIS, ANTINEOPLASTIC agents, INVESTIGATIONAL drugs, NEUTROPENIA, TREATMENT effectiveness, HYPONATREMIA, VOMITING, TREATMENT failure, ANEMIA, MEMBRANE proteins, THROMBOCYTOPENIA, FATIGUE (Physiology), FEMALE reproductive organ tumors, PHARMACODYNAMICS, CHEMICAL inhibitors, EVALUATION

Abstract

Summary: Background Selinexor, a first-in-class, oral selective inhibitor of nuclear export (SINE) compound inhibits Exportin-1(XPO1), had demonstrated synergistic activity with many chemotherapies and conferred in vivo antitumor efficacy in hematologic as well as solid tumors. Methods This open-label, single-center, multi-arm phase 1b study used a standard 3 + 3 design and a "basket type" expansion. Selinexor with intravenous topotecan was given in one of the 13 parallel arms. Patients with advanced or metastatic relapsed/refractory solid tumors following prior systemic therapy, or in whom the addition of selinexor to standard chemotherapy deemed appropriate, were eligible. Results Fourteen patients with the median age of 61 years (range, 22–68years) were treated, and the most common cancer types were gynecological cancers; ovarian (n = 5), endometrial (n = 2), and 1 each with fallopian tube and vaginal cancers. Of the 14 patients treated, 12 (86 %) had at least one treatment-related adverse event (TRAE). The most common TRAEs were anemia (71 %), thrombocytopenia (57 %), hyponatremia (57 %), vomiting (57 %), fatigue (50 %), nausea (50 %), and neutropenia (36 %). Two patients had dose limiting toxicities. One patient dosed at selinexor 80 mg had grade 3 nausea and vomiting and one patient dosed at selinexor 60 mg experienced grade 4 neutropenia and thrombocytopenia. Of the 13 efficacy evaluable patients, one (8 %) with endometrial cancer achieved unconfirmed partial response (uPR) and the time-to-treatment failure (TTF) was 48 weeks, whereas 6 of the 13 (46 %) patients had stable disease (SD) contributing to the clinical benefit rate of 46 %. The median TTF for all patients was 9 weeks (range, 2–48weeks). Conclusions Once weekly selinexor in combination with topotecan was viable and showed some preliminary tumor efficacy. The recommend phase 2 dose of selinexor was 60 mg once weekly in combination with IV topotecan. Trial registration: NCT02419495. Registered 14 April 2015, https://clinicaltrials.gov/ct2/show/NCT02419495 [ABSTRACT FROM AUTHOR]

Published

2021

10. Phase I first-in-human study of HLX07, a novel and improved recombinant anti-EGFR humanized monoclonal antibody, in patients with advanced solid cancers.

Author

Hou, Ming-Mo, Ho, Ching-Liang, Lin, Hsuan-Yu, Zhu, Yunting, and Zhang, Xiaodi

Subjects

EPITHELIAL cell tumors, GENETIC mutation, INTRAVENOUS therapy, NAUSEA, CLINICAL trials, EPIDERMAL growth factor receptors, MONOCLONAL antibodies, PARONYCHIA, TREATMENT effectiveness, VOMITING, TUMORS, FATIGUE (Physiology), PATIENT safety, LONGITUDINAL method, DRUG toxicity

Abstract

Summary: Purpose This study aimed to evaluate the safety and pharmacokinetic (PK) profiles of HLX07, a novel, recombinant, humanized anti-epidermal growth factor receptor (EGFR) antibody, in patients with advanced solid cancers who had failed standard therapy or for whom no standard therapy was available. Methods In this prospective, open-label, Phase I dose escalation study, patients aged ≥18 years (≥20 years for patients in Taiwan) with histologically-confirmed metastatic or recurrent epithelial carcinoma that had no K-RAS or B-RAF mutations were enrolled in a '3 + 3' escalation design. HLX07 was administered weekly by 2-h intravenous infusion at doses ranging from 50 to 800 mg. The primary endpoint was summary listing of participants reporting treatment-emergent adverse events (TEAEs). Secondary endpoints included PK analysis, serum anti-HLX07 antibody assessments and efficacy. Results In total, 19 patients were enrolled between 1 October 2016 and 16 July 2019 to receive HLX07 at doses of 50 (n = 3), 100 (n = 3), 200 (n = 3), 400 (n = 3), 600 (n = 3) and 800 (n = 4) mg per week. All patients experienced at least one TEAE, most commonly fatigue (68.4%), nausea (47.4%), paronychia (31.6%) and vomiting (31.6%). Serious TEAEs were reported in 11 patients but only one serious TEAE (dyspnea in 600 mg cohort) was regarded as possibly related to study treatment. No dose limiting toxicity (DLT) was reported. Systemic exposure to HLX07 increased proportionally with dose. Anti-HLX07 antibodies were not detected in any patients. Conclusion HLX07 was well tolerated (at dose levels up to 800 mg/week) and promising in patients with advanced solid cancers. Clinical Trial Registration: The study was registered at ClinicalTrials.gov: NCT02648490 (Jan 7, 2016). [ABSTRACT FROM AUTHOR]

Published

2021

11. Phase IB study of sorafenib and evofosfamide in patients with advanced hepatocellular and renal cell carcinomas (NCCTG N1135, Alliance).

Author

Tran, Nguyen H, Foster, Nathan R, Mahipal, Amit, Byrne, Thomas, Hubbard, Joleen, Silva, Alvin, Mody, Kabir, Alberts, Steven, and Borad, Mitesh J.

Subjects

THERAPEUTIC use of antineoplastic agents, RENAL cell carcinoma, HYPERTENSION, HAND-foot syndrome, COMBINATION drug therapy, PRODRUGS, DRUG dosage, MUCOSITIS, NAUSEA, ORAL drug administration, EXANTHEMA, IMIDAZOLES, CANCER patients, VOMITING, SORAFENIB, FATIGUE (Physiology), DRUG side effects, HEPATOCELLULAR carcinoma, HYPOXEMIA, DRUG toxicity, LIVER failure

Abstract

Summary: Background Sorafenib (Sor) remains a first-line option for hepatocellular carcinoma (HCC) or refractory renal cell carcinomas (RCC). PLC/PRF/5 HCC model showed upregulation of hypoxia with enhanced efficacy when Sor is combined with hypoxia-activated prodrug evofosfamide (Evo). Methods This phase IB 3 + 3 design investigated 3 Evo dose levels (240, 340, 480 mg/m2 on days 8, 15, 22), combined with Sor 200 mg orally twice daily (po bid) on days 1–28 of a 28-day cycle. Primary objectives included determining maximum tolerated dose (MTD) and recommended phase II dose (RP2D) of Sor + Evo. Results Eighteen patients were enrolled (median age 62.5 years; 17 male /1 female; 12 HCC/6 RCC) across three dose levels (DL0: Sor 200 mg bid/Evo 240 mg/m2 [n = 6], DL1:Sor 200 mg bid/Evo 480 mg/m2 [n = 5], DL1a: Sor 200 mg bid/Evo 340 mg/m2 [n = 7]). Two dose-limiting toxicities (DLTs) were reported with Evo 480 mg/m2 (grade 3 mucositis, grade 4 hepatic failure). Grade 3 rash DLT was observed in one patient at Evo 240 mg/m2. No DLTs were observed at Evo 340 mg/m2. MTD and RP2D were established as Sor 200 mg/Evo 340 mg/m2 and Sor 200/Evo 240 mg/m2, respectively. The most common treatment-related adverse events included fatigue, hand-foot syndrome, hypertension, and nausea/vomiting. Two partial responses were observed, one each at DL0 and DL1a.; disease control rate was 55%. Conclusions RP2D was established as sorafenib 200 mg bid + Evo 240 mg/m2. While preliminary anti-tumor activity was observed, future development must account for advances in immunotherapy in HCC/RCC. [ABSTRACT FROM AUTHOR]

Published

2021

12. Phase 1 cohort expansion study of LY3023414, a dual PI3K/mTOR inhibitor, in patients with advanced mesothelioma.

Author

Zauderer, Marjorie G., Alley, Evan W., Bendell, Johanna, Capelletto, Enrica, Bauer, Todd M., Callies, Sophie, Szpurka, Anna M., Kang, Suhyun, Willard, Melinda D., Wacheck, Volker, and Varghese, Anna M.

Subjects

MESOTHELIOMA, APPETITE, DRUG tolerance, CLINICAL trials, NAUSEA, DIARRHEA, PHOSPHOTRANSFERASES, SIGNAL peptides, ANTINEOPLASTIC agents, LUNG tumors, PERITONEUM tumors, VOMITING, DOSE-effect relationship in pharmacology, DESCRIPTIVE statistics, TUMOR markers, ODDS ratio, FATIGUE (Physiology), LONGITUDINAL method, PATIENT safety, PHARMACODYNAMICS, CHEMICAL inhibitors

Abstract

Summary: BACKGROUND LY3023414 is a selective, ATP competitive inhibitor of class I PI3K isoforms, mTORC1/2 and DNA-PK. A Phase 1 dose escalation, 200 mg twice daily (BID) of LY3023414 was the determined recommended phase 2 dose (RP2D). We report the antitumor activity and safety of LY3023414 monotherapy in patients with advanced mesothelioma.METHODS Patients enrolled had advanced malignant pleural or peritoneal mesothelioma with measurable disease, ECOG PS 0–1, were refractory or ineligible to receive standard therapies. Patients received LY3023414 200 mg BID. This dose expansion cohort is intended to evaluate preliminary antitumor activity of LY3023414 by overall response rate. Safety, tolerability and pharmacokinetics were assessed. Biomarkers associated with treatment response was an exploratory endpoint. RESULTS Forty-two patients received LY3023414 for a median duration of 11.2 weeks (range: 1.1–53.0). One patient had a confirmed partial response (PR) (ORR 2.4%). Three patients had an unconfirmed PR. Seventeen patients had stable disease (SD) (DCR 43%). Most common adverse events (AEs) included fatigue (43%), nausea (43%), decreased appetite (38%), vomiting (33%), and diarrhea (29%). AEs were mostly mild or moderate. Grade ≥ 3 AEs were reported for 21% of patients with fatigue as the most frequent event (10%). Alterations of BAP1 were identified in 11/19 patients as the most common molecular aberration, followed by SETD2 and NF2 alterations. No obvious pattern of genetic changes/mutations in single genes or pathways was associated with anti-tumor activity. CONCLUSION LY3023414 monotherapy (200 mg BID) demonstrated an acceptable and manageable safety profile with limited single-agent activity in patients with advanced mesothelioma. ClinicalTrials.gov identifier: NCT01655225; Date of registration: 19 July 2012. [ABSTRACT FROM AUTHOR]

Published

2021

13. LY3022855, an anti–colony stimulating factor-1 receptor (CSF-1R) monoclonal antibody, in patients with advanced solid tumors refractory to standard therapy: phase 1 dose-escalation trial.

Author

Dowlati, Afshin, Harvey, R. Donald, Carvajal, Richard D., Hamid, Omid, Klempner, Samuel J., Kauh, John Sae Wook, Peterson, Daniel A., Yu, Danni, Chapman, Sonya C., Szpurka, Anna M., Carlsen, Michelle, Quinlan, Tonya, and Wesolowski, Robert

Subjects

THERAPEUTIC use of monoclonal antibodies, LIPASES, DRUG tolerance, CLINICAL trials, INTRAVENOUS therapy, RHABDOMYOLYSIS, NAUSEA, DIARRHEA, FEVER, LEFT ventricular dysfunction, MONOCLONAL antibodies, COMPARATIVE studies, VOMITING, AMYLASES, DOSE-effect relationship in pharmacology, ANEMIA, LACTATE dehydrogenase, TUMORS, DRUG side effects, PANCREATITIS, FATIGUE (Physiology), ANOREXIA nervosa, ACUTE kidney failure

Abstract

Summary: Background Tumor-associated macrophages (TAMs) promote tumor growth, metastasis, and therapeutic resistance via colony-stimulating factor-1 (CSF-1), acting through CSF-1 receptor (CSF-1R) signaling. This phase 1 study determined the safety, tolerability, pharmacokinetics-pharmacodynamics, immunogenicity, and efficacy of the anti–CSF-1R antibody LY3022855 in solid tumors. Methods Patients with advanced solid tumors refractory to standard therapy were enrolled and treated in 2 dosing cohorts: weight-based (part A) and non–weight-based (part B). Part A patients were assigned to intravenous (IV) dose-escalation cohorts: 2.5 mg/kg once per week (QW), 0.3 mg/kg QW, 0.6 mg/kg QW, 1.25 mg/kg once every 2 weeks (Q2W) and 1.25 mg/kg QW doses of LY3022855. Non–weight-based doses in part B were 100 mg and 150 mg IV QW. Results Fifty-two patients (mean age 58.6 ± 10.4 years) were treated with ≥1 dose of LY3022855 (range: 4–6). Five dose-limiting toxicities (left ventricular dysfunction, anemia, pancreatitis, rhabdomyolysis, and acute kidney injury) occurred in 4 patients. The non–weight-based 100 mg QW dose was established as the RP2D. The most common treatment-emergent adverse events were increase in liver function variables, fatigue, nausea, vomiting, diarrhea, anorexia, pyrexia, increased lipase, amylase, and lactate dehydrogenase. Clearance decreased with increasing dose and weight-based dosing had minimal effect on pharmacokinetics. Serum CSF-1, and IL-34 levels increased at higher doses and more frequent dosing, whereas TAMs and CD14dimCD16bright levels decreased. Three patients achieved stable disease. No responses were seen. Conclusions LY3022855 was well tolerated and showed dose-dependent pharmacokinetics-pharmacodynamics and limited clinical activity in a heterogenous solid tumor population. ClinicalTrials.gov IDNCT01346358 (Registration Date: May 3, 2011). [ABSTRACT FROM AUTHOR]

Published

2021

14. Phase 1 dose-escalation study of a novel oral PI3K/mTOR dual inhibitor, LY3023414, in patients with cancer.

Author

Kondo, Shunsuke, Tajimi, Masaomi, Funai, Tomohiko, Inoue, Koichi, Asou, Hiroya, Ranka, Vinay Kumar, Wacheck, Volker, and Doi, Toshihiko

Subjects

THERAPEUTIC use of antineoplastic agents, ANTINEOPLASTIC agents, APPETITE, CLINICAL trials, DIARRHEA, DOSE-effect relationship in pharmacology, ENZYME inhibitors, HYPERGLYCEMIA, NAUSEA, PROTEIN kinases, PYRIDINE, QUINOLONE antibacterial agents, STOMATITIS, TUMORS, HYPOPHOSPHATEMIA, PROTEIN kinase inhibitors, PLATELET count, CHEMICAL inhibitors

Abstract

Summary: LY3023414 is an oral, selective adenosine triphosphate-competitive inhibitor of class I phosphatidylinositol 3-kinase isoforms, mammalian target of rapamycin, and DNA-protein kinase in clinical development. We report results of a 3 + 3 dose-escalation Phase 1 study for twice-daily (BID) dosing of LY3023414 monotherapy in Japanese patients with advanced malignancies. The primary objective was to evaluate tolerability and safety of LY3023414. Secondary objectives were to evaluate pharmacokinetics and to explore antitumor activity. A total of 12 patients were enrolled and received 150 mg (n = 3) or 200 mg (n = 9) LY3023414 BID. Dose-limiting toxicities were only reported at 200 mg LY3023414 for 2 patients with Grade 3 stomatitis. Common treatment-related adverse events (AEs) across both the dose levels included stomatitis (75.0%), nausea (66.7%), decreased appetite (58.3%), diarrhea, and decreased platelet count (41.7%), and they were mostly mild or moderate in severity. Related AEs Grade ≥ 3 reported for ≥1 patient included anemia, stomatitis, hypophosphatemia, and hyperglycemia (n = 2, 16.7%). Two patients discontinued due to AEs (interstitial lung disease and stomatitis). No fatal events were reported. The pharmacokinetic profile of LY3023414 was characterized by rapid absorption and elimination. Five patients had a best overall response of stable disease (150 mg, n = 3; 200 mg, n = 2) for a 55.6% disease control rate. LY3023414 up to 200 mg BID is tolerable and safe in Japanese patients with advanced malignancies. [ABSTRACT FROM AUTHOR]

Published

2020

15. A Canadian cancer trials group phase IB study of durvalumab (anti-PD-L1) plus tremelimumab (anti-CTLA-4) given concurrently or sequentially in patients with advanced, incurable solid malignancies.

Author

Nehra, J., Bradbury, P. A., Ellis, P. M., Laskin, J., Kollmannsberger, C., Hao, D., Juergens, R. A., Goss, G., Wheatley-Price, P., Hotte, S. J., Gelmon, K., Tinker, A. V., Brown-Walker, P., Gauthier, I., Tu, D., Song, X., Khan, A., Seymour, Lesley, and Smoragiewicz, M.

Subjects

COMBINATION drug therapy, EXANTHEMA, FATIGUE (Physiology), ITCHING, MONOCLONAL antibodies, NAUSEA, STATISTICAL sampling, TUMORS, RANDOMIZED controlled trials, TREATMENT effectiveness, DESCRIPTIVE statistics

Abstract

Summary: Background The IND.226 study was a phase Ib study to determine the recommended phase II dose of durvalumab + tremelimumab in combination with standard platinum-doublet chemotherapy. Sequential administration of multiple agents increases total chair time adding costs overall and inconvenience for patients. This cohort of the IND.226 study evaluated the safety and tolerability of durvalumab + tremelimumab given either sequentially (SEQ) or concurrently (CON). Methods Patients with advanced solid tumours were enrolled and randomised to either SEQ tremelimumab 75 mg IV over 1 h followed by durvalumab 1500 mg IV over 1 h q4wks on the same day, or CON administration over 1 h. The serum pharmacokinetic profile of SEQ versus CON of durvalumab and tremelimumab administration was also evaluated. Results 14 patients either received SEQ (n = 7pts) or CON (n = 7 pts). There were no infusion related reactions. Drug related adverse events (AEs) were mainly low grade and manageable, and comparable in frequency between SEQ/CON- fatigue (43%/57%), rash (43%/43%), pruritus (43%/29%) and nausea (14%/29%). One patient in each cohort discontinued treatment due to toxicity. The PK profiles of durvalumab and tremelimumab were similar between CON and SEQ, and to historical reference data. Conclusions Concurrent administration of durvalumab and tremelimumab over 1 h is safe with a comparable PK profile to sequential administration. [ABSTRACT FROM AUTHOR]

Published

2020

16. Epigallocatechin-3-gallate mouthwash protects mucosa from radiation-induced mucositis in head and neck cancer patients: a prospective, non-randomised, phase 1 trial.

Author

Zhu, Wanqi, Mei, Hui, Jia, Li, Zhao, Hanxi, Li, Xiaolin, Meng, Xiangjiao, Zhao, Xianguang, Xing, Ligang, and Yu, Jinming

Subjects

CLINICAL trials, COMBINED modality therapy, COMPARATIVE studies, DRUG dosage, DRUG toxicity, FLAVONOIDS, HEAD tumors, LONGITUDINAL method, MOUTHWASHES, NAUSEA, NECK tumors, ORAL mucosa, RADIATION injuries, RADIOTHERAPY, STOMATITIS, T-test (Statistics), TREATMENT effectiveness, PRE-tests & post-tests, DESCRIPTIVE statistics

Abstract

Summary: Radiation-induced oral mucositis has a dismal outcome with limited treatment options. We conducted a phase I study to evaluate the safety and preliminary efficacy of epigallocatechin-3-gallate (EGCG) mouthwash when given along with radiation in head and neck cancer. Patients with pathologically confirmed head and neck cancer were eligible for this study. EGCG mouthwash was administered at the assigned dosage level (starting at 440 μmol/L, three times a day) in a standard 3 + 3 dose escalation design. Mucosal toxicity, patient satisfaction, and mucositis-related pain (MTP) were assessed weekly. The primary endpoint was safety of EGCG, and the secondary endpoint was to determine the relief of the mucositis symptom. The pre- and post-treatment parameters were compared using the paired t-test. 20 patients were enrolled. The maximum tolerated dose of the EGCG mouthwash was 2200 μmol/L. Burning (n = 1/20) and nausea (n = 3/20) were the most common toxicities. No patients experienced WHO Grade 3 or higher mucositis. MTP scores significantly decreased after EGCG administration over time (p < 0.05). Adding EGCG mouthwash to radiotherapy is feasible without increasing toxicities. The recommended dose for phase II study is determined to be 1760 μmol/L, and EGCG administration reduces radiation-induced oral mucosal injury in patients. [ABSTRACT FROM AUTHOR]

Published

2020

17. A phase 1 study of the MDM2 antagonist RO6839921, a pegylated prodrug of idasanutlin, in patients with advanced solid tumors.

Author

Abdul Razak, Albiruni R., Miller, Wilson H., Uy, Geoffrey L., Blotner, Steven, Young, Anne-Marie, Higgins, Brian, Chen, Lin-Chi, and Gore, Lia

Subjects

CLINICAL trials, CYTOKINES, DOSE-effect relationship in pharmacology, DRUG toxicity, FATIGUE (Physiology), IMIDAZOLES, INTRAVENOUS therapy, NAUSEA, NEUTROPENIA, PRODRUGS, PROTEINS, THROMBOCYTOPENIA, TUMORS, VOMITING, TREATMENT effectiveness, DESCRIPTIVE statistics, CHEMICAL inhibitors, PHARMACODYNAMICS

Abstract

Summary: Purpose MDM2 is a negative regulator of the tumor suppressor p53. RO6839921 is an inactive pegylated prodrug of idasanutlin, an MDM2 antagonist, developed for intravenous administration. On cleavage by plasma esterases, the active principle (AP = idasanutlin) is released. This phase 1 study investigated the safety, pharmacokinetics, and pharmacodynamics of RO6839921 in patients with advanced solid tumors (NCT02098967). Methods Patients were evaluated on a 5-day dosing schedule every 28 days. Dose escalation used the Bayesian new continual reassessment model. Accelerated dose titration was permitted until grade ≥2 drug-related AEs were observed. The target DLT rate to define the MTD was 16–25%. p53 activation was assessed by measuring macrophage inhibitory cytokine-1 (MIC-1). Results Forty-one patients received 14–120 mg AP; 39 were DLT evaluable. The MTD was 110-mg AP (8% DLT rate), whereas 120-mg AP had a 44% DLT rate. DLTs were neutropenia, thrombocytopenia, and stridor. The most common treatment-related AEs (≥30%) were nausea, fatigue, vomiting, and thrombocytopenia. Pharmacokinetic analyses indicated rapid conversion of prodrug to AP and an approximately linear and dose-proportional dose-exposure relationship, with a 2-fold increase in exposure between Days 1 and 5 of AP. MIC-1 increases were exposure dependent. Stable disease was observed in 14 patients (34%). Conclusions RO6839921 showed reduced pharmacokinetic exposure variability and a safety profile comparable with that of oral idasanutlin. Although this study indicated that RO6839921 could be administered to patients, the results did not provide sufficient differentiation or improvement in the biologic or safety profile compared with oral idasanutlin to support continued development. [ABSTRACT FROM AUTHOR]

Published

2020

18. Phase I study of the anti-endothelin B receptor antibody-drug conjugate DEDN6526A in patients with metastatic or unresectable cutaneous, mucosal, or uveal melanoma.

Author

Sandhu, Shahneen, McNeil, Catriona M., LoRusso, Patricia, Patel, Manish R., Kabbarah, Omar, Li, Chunze, Sanabria, Sandra, Flanagan, W. Michael, Yeh, Ru-Fang, Brunstein, Flavia, Nazzal, Denise, Hicks, Rodney, Lemahieu, Vanessa, Meng, Raymond, Hamid, Omid, and Infante, Jeffrey R.

Subjects

BALDNESS, CANCER patients, CELL receptors, CLINICAL trials, DIARRHEA, ENDOTHELINS, INTRAVENOUS therapy, MELANOMA, METASTASIS, MONOCLONAL antibodies, NAUSEA, PERIPHERAL neuropathy, PATIENT safety, UVEA cancer, TREATMENT effectiveness, DESCRIPTIVE statistics, INVESTIGATIONAL drugs, CANCER fatigue, PHARMACODYNAMICS

Abstract

Summary: Background Endothelin B receptor (ETBR) is involved in melanoma pathogenesis and is overexpressed in metastatic melanoma. The antibody-drug conjugate DEDN6526A targets ETBR and is comprised of the humanized anti-ETBR monoclonal antibody conjugated to the anti-mitotic agent monomethyl auristatin E (MMAE). Methods This Phase I study evaluated the safety, pharmacokinetics, pharmacodynamics, and anti-tumor activity of DEDN6526A (0.3–2.8 mg/kg) given every 3 weeks (q3w) in patients with metastatic or unresectable cutaneous, mucosal, or uveal melanoma. Results Fifty-three patients received a median of 6 doses of DEDN6526A (range 1–49). The most common drug-related adverse events (>25% across dose levels) were fatigue, peripheral neuropathy, nausea, diarrhea, alopecia, and chills. Three patients in dose-escalation experienced a dose-limiting toxicity (infusion-related reaction, increased ALT/AST, and drug-induced liver injury). Based on cumulative safety data across all dose levels, the recommended Phase II dose (RP2D) for DEDN6526A was 2.4 mg/kg intravenous (IV) q3w. The pharmacokinetics of antibody-conjugated MMAE and total antibody were dose-proportional at doses ranging from 1.8–2.8 mg/kg. A trend toward faster clearance was observed at doses of 0.3–1.2 mg/kg. There were 6 partial responses (11%) in patients with metastatic cutaneous or mucosal melanoma, and 17 patients (32%) had prolonged stable disease ≥6 months. Responses were independent of BRAF mutation status but did correlate with ETBR expression. Conclusion DEDN6526A administered at the RP2D of 2.4 mg/kg q3w had an acceptable safety profile and showed evidence of anti-tumor activity in patients with cutaneous, mucosal, and uveal melanoma. ClinicalTrials.gov identifier: NCT01522664. [ABSTRACT FROM AUTHOR]

Published

2020

19. A phase Ib study of GSK3052230, an FGF ligand trap in combination with pemetrexed and cisplatin in patients with malignant pleural mesothelioma.

Author

van Brummelen, Emilie M. J., Levchenko, Evgeny, Dómine, Manuel, Fennell, Dean A., Kindler, Hedy L., Viteri, Santiago, Gadgeel, Shirish, López, Pilar Garrido, Kostorov, Vladimir, Morgensztern, Daniel, Orlov, Sergey, Zauderer, Marjorie G., Vansteenkiste, Johan F., Baker-Neblett, Katherine, Vasquez, James, Wang, Xiaowei, Bellovin, David I., Schellens, Jan H. M., Yan, Li, and Mitrica, Ionel

Subjects

ANTINEOPLASTIC agents, APPETITE, CELL receptors, COMBINATION drug therapy, CISPLATIN, CLINICAL trials, CONFIDENCE intervals, DRUG dosage, DRUG toxicity, FATIGUE (Physiology), FIBROBLASTS, GROWTH factors, MEDICAL cooperation, MESOTHELIOMA, NAUSEA, NEUTROPHILS, RESEARCH, PLEURAL tumors, ADVERSE health care events, PEMETREXED, HYPERPHOSPHATEMIA

Abstract

Summary: Background Fibroblast growth factors (FGFs) have a fundamental role in cancer. Sequestering FGFs with GSK3052230 (FP-1039) blocks their ability to activate FGFRs while avoiding toxicities associated with small molecule inhibitors of FGFR, including hyperphosphatemia and retinal, nail, and skin toxicities. Methods A multicenter, open-label, phase Ib study evaluated weekly GSK3052230 added to pemetrexed/cisplatin in patients with treatment-naive, unresectable malignant pleural mesothelioma. Doses were escalated according to a 3 + 3 design, followed by cohort expansion at the maximum tolerated dose (MTD). Endpoints included safety, overall response rate, progression-free survival, and pharmacokinetics. Results 36 patients were dosed at 10, 15, and 20 mg/kg doses of GSK3052230. Three dose-limiting toxicities were observed at 20 mg/kg and one at 15 mg/kg. The MTD was defined as 15 mg/kg and used for cohort expansion. The most common treatment-related adverse events (AEs) were nausea (56%), decreased appetite (36%), infusion reactions (36%), decreased neutrophil counts (36%), and fatigue (33%). The confirmed ORR was 39% (95% CI: 23.1–56.5) (14/36 PRs) and 47% had stable disease (17/36), giving a disease control rate of 86%. At 15 mg/kg GSK3052230 (n = 25), the ORR was 44% (95% CI: 24.4–65.1), and the median PFS was 7.4 months (95% CI: 6.7–13.4). Four patients had disease control for over 1 year, and three were still ongoing. Conclusion At 15 mg/kg weekly, GSK3052230 was well tolerated in combination with pemetrexed/cisplatin and durable responses were observed. Importantly, AEs associated with small molecule inhibitors of FGFR were not observed, as predicted by the unique mechanism of action of this drug. [ABSTRACT FROM AUTHOR]

Published

2020

20. Phase Ib study of the MEK inhibitor cobimetinib (GDC-0973) in combination with the PI3K inhibitor pictilisib (GDC-0941) in patients with advanced solid tumors.

Author

Shapiro, Geoffrey I., LoRusso, Patricia, Kwak, Eunice, Pandya, Susan, Rudin, Charles M., Kurkjian, Carla, Cleary, James M., Pilat, Mary Jo, Jones, Suzanne, de Crespigny, Alex, Fredrickson, Jill, Musib, Luna, Yan, Yibing, Wongchenko, Matthew, Hsieh, Hsin-Ju, Gates, Mary R., Chan, Iris T., and Bendell, Johanna

Subjects

ALLERGIES, ANTINEOPLASTIC agents, CLINICAL trials, DEHYDRATION, DIARRHEA, DRUG side effects, CLINICAL drug trials, EXANTHEMA, FATIGUE (Physiology), LONGITUDINAL method, GENETIC mutation, NAUSEA, HEALTH outcome assessment, PROTEIN kinases, STOMATITIS, TASTE disorders, TIME, TUMORS, VOMITING, DESCRIPTIVE statistics

Abstract

Summary: Purpose We investigated the combination of the MEK inhibitor, cobimetinib, and the pan-PI3K inhibitor, pictilisib, in an open-label, phase Ib study. Experimental Design Patients with advanced solid tumors were enrolled in 3 dose escalation schedules: (1) both agents once-daily for 21-days-on 7-days-off ("21/7"); (2) intermittent cobimetinib and 21/7 pictilisib ("intermittent"); or (3) both agents once-daily for 7-days-on 7-days-off ("7/7"). Starting doses for the 21/7, intermittent, and 7/7 schedules were 20/80, 100/130, and 40/130 mg of cobimetinib/pictilisib, respectively. Nine indication-specific expansion cohorts interrogated the recommended phase II dose and schedule. Results Of 178 enrollees (dose escalation: n = 98), 177 patients were dosed. The maximum tolerated doses for cobimetinib/pictilisib (mg) were 40/100, 125/180, and not reached, for the 21/7, intermittent, and 7/7 schedules, respectively. Six dose-limiting toxicities included grade 3 (G3) elevated lipase, G4 elevated creatine phosphokinase, and G3 events including fatigue concurrent with a serious adverse event (SAE) of diarrhea, decreased appetite, and SAEs of hypersensitivity and dehydration. Common drug-related adverse events included nausea, fatigue, vomiting, decreased appetite, dysgeusia, rash, and stomatitis. Pharmacokinetic parameters of the drugs used in combination were unaltered compared to monotherapy exposures. Confirmed partial responses were observed in patients with BRAF-mutant melanoma (n = 1) and KRAS-mutant endometrioid adenocarcinoma (n = 1). Eighteen patients remained on study ≥6 months. Biomarker data established successful blockade of MAP kinase (MAPK) and PI3K pathways. The metabolic response rate documented by FDG-PET was similar to that observed with cobimetinib monotherapy. Conclusions Cobimetinib and pictilisib combination therapy in patients with solid tumors had limited tolerability and efficacy. [ABSTRACT FROM AUTHOR]

Published

2020

21. A phase I study to determine the maximum tolerated dose of trifluridine/tipiracil and oxaliplatin in patients with refractory metastatic colorectal cancer: LUPIN study.

Author

Suenaga, Mitsukuni, Wakatsuki, Takeru, Mashima, Tetsuo, Ogura, Mariko, Ichimura, Takashi, Shinozaki, Eiji, Nakayama, Izuma, Osumi, Hiroki, Ota, Yumiko, Takahari, Daisuke, Chin, Keisho, Seimiya, Hiroyuki, and Yamaguchi, Kensei

Subjects

ANOREXIA nervosa, COLON tumors, DRUG dosage, DRUG toxicity, HETEROCYCLIC compounds, METASTASIS, NAUSEA, NEUTROPENIA, RECTUM tumors, THROMBOCYTOPENIA, OXALIPLATIN, DISEASE progression, TREATMENT delay (Medicine)

Abstract

Summary: Background The effectiveness of reintroducing oxaliplatin for metastatic colorectal cancer (mCRC) refractory to both oxaliplatin and irinotecan was previously reported in a phase II study (RE-OPEN). We conducted a phase I study to determine the maximum tolerated dose of oxaliplatin plus trifluridine/tipiracil (FTD/TPI) in patients with refractory mCRC. Patients and Methods Three dosages of intravenous oxaliplatin (50, 65 and 85 mg/m2) on days 1 and 15 and a fixed dose of FTD/TPI 35 mg/m2 twice daily (bid) on days 1–5 and 15–19 every 4 weeks were investigated in patients with refractory mCRC using a 3 + 3 design. Eligible patients had received prior oxaliplatin-based treatment that achieved a response or stable disease followed by confirmed disease progression at least 6 months before entering the study. Results Twelve patients were enrolled in the study. Three of six patients in the oxaliplatin 85 mg/m2 cohort had dose-limiting toxicities (DLTs) with treatment delays during the second cycle at ≥8 days due to grade ≥ 2 neutropenia or grade 2 AST/ALT increased. No DLTs were observed in the other cohorts. Grade ≥ 3 AEs were neutropenia (n = 3), thrombocytopenia (n = 1), anorexia (n = 1), and nausea (n = 1). There was no evidence of allergic reaction to oxaliplatin or severe peripheral sensory neuropathy. Conclusions A combination of FTD/TPI 35 mg/m2 bid on days 1–5 and 15–19 and oxaliplatin 85 mg/m2 on days 1 and 15 every 4 weeks could be a suitable regimen for the recommended dose of FTD/TPI plus oxaliplatin in patients with refractory mCRC. [ABSTRACT FROM AUTHOR]

Published

2020

22. First-in-human study of IM156, a novel potent biguanide oxidative phosphorylation (OXPHOS) inhibitor, in patients with advanced solid tumors

Author

Filip Janku, Seung-Hoon Beom, Yong Wha Moon, Tae Won Kim, Young G. Shin, Dong-Seok Yim, Gun Min Kim, Hyo Song Kim, Sun Young Kim, Jae-Ho Cheong, Young Woo Lee, Barb Geiger, Sanghee Yoo, Archie Thurston, Dean Welsch, Marc S. Rudoltz, and Sun Young Rha

Subjects

Pharmacology, Dose-Response Relationship, Drug, Maximum Tolerated Dose, Oncology, Neoplasms, Biguanides, Humans, Antineoplastic Agents, Nausea, Pharmacology (medical), Oxidative Phosphorylation

Abstract

Preclinical models suggest anticancer activity of IM156, a novel biguanide mitochondrial protein complex 1 inhibitor of oxidative phosphorylation (OXPHOS). This first-in-human dose-escalation study enrolled patients with refractory advanced solid tumors to determine the maximum tolerated dose (MTD) or recommended phase 2 dose (RP2D). Eligible patients received oral IM156 every other day (QOD) or daily (QD) and were assessed for safety, dose-limiting toxicities (DLTs), pharmacokinetics, and preliminary signals of efficacy. 22 patients with advanced cancers (gastric, n = 8; colorectal, n = 3; ovarian, n = 3; other, n = 8) received IM156 100 to 1,200 mg either QOD or QD. There were no DLTs. However, 1,200 mg QD was not well tolerated due to nausea; 800 mg QD was determined as the RP2D. The most frequent treatment-related AEs (TRAEs) were nausea (n = 15; 68%), diarrhea (n = 10; 46%), emesis (n = 9; 41%), fatigue (n = 4; 18%) and abdominal pain, constipation, and blood lactate increased (n = 2 each; 9%). Grade 3 nausea (n = 3; 14%) was the only grade ≥ 3 TRAE. Plasma exposures increased dose proportionally; mean Day 27 area under the curve (AUC0-24) values were higher following QD administration compared to the respective QOD regimen. Stable disease (SD), observed in 7 (32%) patients (confirmed in 2 [9%]), was the best response. To our knowledge, this is the first phase 1 study of an OXPHOS inhibitor that established a RP2D for further clinical development in cancer. Observed AEs of IM156 were manageable and SD was the best response.

Published

2022

23. A phase 2, open-label study of brentuximab vedotin in patients with CD30-expressing solid tumors.

Author

Sharman, Jeffrey P., Wheler, Jennifer J., Einhorn, Lawrence, Dowlati, Afshin, Shapiro, Geoffrey I., Hilton, John, Burke, John M., Siddiqi, Tanya, Whiting, Nancy, and Jalal, Shadia I.

Subjects

ANTIGENS, ANTINEOPLASTIC agents, APPETITE, CELL lines, CLINICAL trials, DOSE-effect relationship in pharmacology, DRUG toxicity, FATIGUE (Physiology), LYMPHOMAS, MONOCLONAL antibodies, NAUSEA

Abstract

Summary: Purpose Brentuximab vedotin (BV) is an anti-CD30 antibody-drug conjugate used in the treatment of several types of lymphomas. Expression of the target antigen has also been reported on a variety of malignant tumors of nonlymphoid origin. This phase 2, open-label study evaluated the safety and antitumor activity of BV in patients with CD30-expressing nonlymphomatous malignancies. Methods Patients were dosed with 1.8 or 2.4 mg/kg BV once every three weeks. Antitumor activity was assessed at Cycles 2, 4, and every 4 cycles thereafter. Patients with stable disease or better were eligible to continue treatment until disease progression, unacceptable toxicity, or study closure. Results Of the 2693 patients screened, 3.8% had solid tumors with CD30 expression and 63 eligible patients with solid tumors enrolled in this study. The most common CD30 positive solid tumors were testicular cancer and mesothelioma. Both subtypes had more than one patient with an objective response. The median duration of BV exposure was 6.1 weeks. The disease control rate, defined as achieving stable disease or better at any point during the study, was 55%. The objective response rate was 11%, with a median duration of response of 2.92 months. The most common adverse events reported were fatigue (57%), nausea (33%), and decreased appetite (32%). Conclusion The safety profile of BV in patients with solid tumors was similar to the known safety profile of BV. In solid tumors, BV had modest activity as a single agent, which was similar to other second-line treatments already available to patients. [ABSTRACT FROM AUTHOR]

Published

2019

24. A phase I study of the vascular endothelial growth factor inhibitor Vatalanib in combination with Pemetrexed disodium in patients with advanced solid tumors.

Author

Wang, Fen, Molina, Julian, Satele, Daniel, Yin, Jun, Lim, Vun-Sin, and Adjei, Alex A.

Subjects

ANOREXIA nervosa, ANTINEOPLASTIC agents, CANCER patients, CLINICAL trials, CONSTIPATION, DEHYDRATION, DIARRHEA, DRUG tolerance, DRUG dosage, DRUG toxicity, FATIGUE (Physiology), FEBRILE neutropenia, NAUSEA, PATIENT safety, STOMATITIS, THROMBOCYTOPENIA, TUMORS, VOMITING, VASCULAR endothelial growth factors, TREATMENT effectiveness, DESCRIPTIVE statistics, PEMETREXED, PHARMACODYNAMICS

Abstract

Summary: Introduction Vatalanib is an oral receptor tyrosine kinase inhibitor that blocks all known VEGF, PDGF, and c-Kit receptors. This phase I study evaluated the safety, tolerability, and biologic activity of the combination of vatalanib with pemetrexed disodium in patients with advanced solid tumors. Methods Patients were administered escalating twice daily doses of vatalanib in combination with pemetrexed disodium in 21-day cycles. A dose expansion cohort was enrolled to further define the maximum tolerated dose (MTD) and further evaluate efficacy. Results A total of 29 patients were enrolled in the study (dose escalation, 9; dose expansion, 20). Dose-limiting toxicities included grade 4 thrombocytopenia (6.9%) and febrile neutropenia, anorexia, constipation, and dehydration. Other common adverse events were fatigue (75%), nausea (66%), vomiting (48%), oral mucositis (31%) and diarrhea (28%). The majority of these toxicities were Grade 1–2. The MTD was reached at vatalanib 250 mg twice daily continuously combined with pemetrexed disodium 500 mg/m2 day 1. Overall, 2 patients (6.9%) had partial responses, 8 (27.6%) had stable disease for at least 4 cycles, 5 had progressive disease (17.2%) and 5 went off study before disease assessment. Conclusion The combination of vatalanib with pemetrexed disodium was feasible, but not well tolerated. The modest efficacy results are consistent with other results obtained from combinations of chemotherapy and a large number of VEGF tyrosine kinase inhibitors. This combination should not be developed further unless predictive biomarkers can be identified. [ABSTRACT FROM AUTHOR]

Published

2019

25. Switch maintenance therapy with S-1 after induction therapy with carboplatin and nanoparticle albumin-bound paclitaxel in advanced lung squamous cell carcinoma.

Author

Akiyama, Norimichi, Karayama, Masato, Inui, Naoki, Yasui, Hideki, Hozumi, Hironao, Suzuki, Yuzo, Furuhashi, Kazuki, Fujisawa, Tomoyuki, Enomoto, Noriyuki, Nakamura, Yutaro, Inami, Nao, Matsuura, Shun, Kaida, Yusuke, Uto, Tomohiro, Matsui, Takashi, Asada, Kazuhiro, Matsuda, Hiroyuki, Fujii, Masato, Toyoshima, Mikio, and Suda, Takafumi

Subjects

THERAPEUTIC use of antimetabolites, ANTIMETABOLITES, ANTINEOPLASTIC agents, CANCER patients, CLINICAL trials, CONFIDENCE intervals, DIARRHEA, DRUG toxicity, LUNG tumors, NANOPARTICLES, NAUSEA, NEUTROPENIA, ORAL drug administration, PACLITAXEL, SAFETY, SQUAMOUS cell carcinoma, SURVIVAL analysis (Biometry), ALBUMINS, TREATMENT effectiveness, DISEASE progression, TREATMENT duration, DESCRIPTIVE statistics, CARBOPLATIN

Abstract

Summary: Background Optimal maintenance therapy for lung squamous cell carcinoma (SCC) has not been established. The aim of this study was to evaluate the efficacy and safety of switch maintenance therapy with S-1, an oral fluoropyrimidine, after induction therapy with carboplatin and nanoparticle albumin-bound paclitaxel (nab-paclitaxel) in chemotherapy-naïve patients with advanced SCC. Methods Chemotherapy-naïve patients with advanced SCC received induction therapy with four cycles of carboplatin (at an area under the curve of 6, day 1 of a 28-day cycle) and nab-paclitaxel (100 mg/kg, days 1, 8, and 15). Patients who achieved disease control after induction therapy received maintenance therapy with S-1 (80 mg/m2, days 1–14 of a 21-day cycle) until disease progression or unacceptable toxicity. The primary endpoint was progression-free survival (PFS) from the start of maintenance therapy. Results Seventy-two patients with SCC were enrolled to the study. After four cycles of induction therapy, 35 (48.6%) patients achieved disease control, and 31 (43.1%) of these patients received maintenance therapy. Median PFS from the start of maintenance therapy was 3.0 months (95% confidence interval: 2.1–3.8 months). The most common toxicities of grade 3 or higher during maintenance therapy were nausea (13.3%), neutropenia (10.0%), and diarrhea (6.7%). Conclusions Switch maintenance therapy with S-1 after induction therapy with carboplatin and nab-paclitaxel was associated with moderate efficacy and acceptable safety and may represent a feasible treatment option for patients with advanced SCC. [ABSTRACT FROM AUTHOR]

Published

2019

26. Phase 1 dose-escalation study of momelotinib, a Janus kinase 1/2 inhibitor, combined with gemcitabine and nab-paclitaxel in patients with previously untreated metastatic pancreatic ductal adenocarcinoma.

Author

Ng, Kimmie, Hendifar, Andrew, Starodub, Alexander, Chaves, Jorge, Yang, Yingsi, Koh, Brian, Barbie, David, Hahn, William C., and Fuchs, Charles S.

Subjects

THERAPEUTIC use of antimetabolites, ADENOCARCINOMA, ANEMIA, ANTIMETABOLITES, ANTINEOPLASTIC agents, CANCER cells, CLINICAL trials, DRUG tolerance, DRUG dosage, DRUG side effects, CLINICAL drug trials, DRUG toxicity, FATIGUE (Physiology), METASTASIS, NAUSEA, NEUROTRANSMITTER uptake inhibitors, NEUTROPENIA, PACLITAXEL, PANCREATIC tumors, TREATMENT effectiveness, JANUS kinases, PHARMACODYNAMICS, THERAPEUTICS

Abstract

Purpose Preclinical evidence suggests the importance of Janus activating kinase (JAK) and TANK-binding kinase 1 (TBK1) in pancreatic ductal adenocarcinoma (PDAC). We evaluated the safety and efficacy of momelotinib (MMB), a JAK1/2 inhibitor with additional activity against TBK1, plus albumin-bound paclitaxel + gemcitabine (nab-P + G), in patients with previously untreated metastatic PDAC. Experimental Design Patients were enrolled into five cohorts of increasing doses of MMB between 100 and 200 mg administered once or twice daily in combination with nab-P + G in 28-day cycles to determine maximum tolerated dose (MTD). Safety, efficacy, pharmacokinetics, and pharmacodynamics were assessed for all patients. Results Twenty-five patients were enrolled. Dose-limiting toxicities of Grade 3 diarrhea occurred in 1 patient each in the 100 and 200 mg MMB once-daily dose groups. MTD was not reached. The 200 mg MMB twice-daily was the maximum administered dose. Objective response rate was 28% (all partial responses), and 13 (52%) patients had a best response of stable disease. The most common adverse events (AEs) were fatigue (80%), nausea (76%), and anemia (68%). Grade 3 or 4 AEs, most commonly neutropenia (32%), were reported by 88% of patients, of which 44% were considered related to MMB. Pharmacokinetic analyses showed MMB concentrations were too low for TBK1 inhibition. Conclusions MMB was safe and well tolerated in combination with nab-P + G. As no OS or PFS benefit vs nab-P + G was apparent in context of suboptimal engagement of the target TBK1, this study does not support further development of MMB as a first-line therapy in pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2019

27. Phase Ib study of pevonedistat, a NEDD8-activating enzyme inhibitor, in combination with docetaxel, carboplatin and paclitaxel, or gemcitabine, in patients with advanced solid tumors.

Author

Lockhart, A Craig, Bauer, Todd M., Aggarwal, Charu, Lee, Carrie B., Harvey, R Donald, Cohen, Roger B., Sedarati, Farhad, Nip, Tsz Keung, Faessel, Hélène, Dash, Ajeeta B., Dezube, Bruce J., Faller, Douglas V., and Dowlati, Afshin

Subjects

ANTINEOPLASTIC agents, DOCETAXEL, THERAPEUTIC use of antimetabolites, CANCER chemotherapy, CLINICAL trials, DRUG dosage, DRUG side effects, DRUG toxicity, FATIGUE (Physiology), ENZYME inhibitors, FEBRILE neutropenia, LIVER diseases, LONGITUDINAL method, MEDICAL quality control, NAUSEA, THROMBOCYTOPENIA, PACLITAXEL, TRANSCRIPTION factors, TUMORS, TUMOR classification, TERMINATION of treatment, TREATMENT effectiveness, CARBOPLATIN, INVESTIGATIONAL drugs, THERAPEUTICS

Abstract

Purpose This phase Ib study (NCT01862328) evaluated the maximum tolerated dose (MTD), safety, and efficacy of pevonedistat in combination with standard-of-care chemotherapies in patients with solid tumors. Methods Patients received pevonedistat with docetaxel (arm 1, n = 22), carboplatin plus paclitaxel (arm 2, n = 26), or gemcitabine (arm 3, n = 10) in 21-days (arms 1 and 2) or 28-days (arm 3) cycles. A lead-in cohort (arm 2a, n = 6) determined the arm 2 carboplatin dose. Dose escalation proceeded via continual modified reassessment. Results Pevonedistat MTD was 25 mg/m2 (arm 1) or 20 mg/m2 (arm 2); arm 3 was discontinued due to poor tolerability. Fifteen (23%) patients experienced dose-limiting toxicities during cycle 1 (grade ≥3 liver enzyme elevations, febrile neutropenia, and thrombocytopenia), managed with dose holds or reductions. Drug-related adverse events (AEs) occurred in 95% of patients. Most common AEs included fatigue (56%) and nausea (50%). One drug-related death occurred in arm 3 (febrile neutropenia). Pevonedistat exposure increased when co-administered with carboplatin plus paclitaxel; no obvious changes were observed when co-administered with docetaxel or gemcitabine. Among 54 response-evaluable patients, two had complete responses (arm 2) and 10 had partial responses (three in arm 1, one in arm 2a, six in arm 2); overall response rates were 16% (arm 1) and 35% (arm 2). High ERCC1 expression correlated with clinical benefit in arm 2. Conclusion Pevonedistat with docetaxel or with carboplatin plus paclitaxel was tolerable without cumulative toxicity. Sustained clinical responses were observed in pretreated patients receiving pevonedistat with carboplatin and paclitaxel. ClinicalTrials.gov identifier: NCT01862328. [ABSTRACT FROM AUTHOR]

Published

2019

28. Eftozanermin alfa (ABBV-621) monotherapy in patients with previously treated solid tumors: findings of a phase 1, first-in-human study

Author

Patricia LoRusso, Mark J. Ratain, Toshihiko Doi, Drew W. Rasco, Maja J. A. de Jonge, Victor Moreno, Benedito A. Carneiro, Lot A. Devriese, Adam Petrich, Dimple Modi, Susan Morgan-Lappe, Silpa Nuthalapati, Monica Motwani, Martin Dunbar, Jaimee Glasgow, Bruno C. Medeiros, Emiliano Calvo, and Medical Oncology

Subjects

Pharmacology, SDG 3 - Good Health and Well-being, Dose-Response Relationship, Drug, Maximum Tolerated Dose, Oncology, Neoplasms, Humans, Antineoplastic Agents, Nausea, Pharmacology (medical), Fatigue

Abstract

Eftozanermin alfa (eftoza), a second-generation tumor necrosis factor-related apoptosis-inducing ligand receptor (TRAIL-R) agonist, induces apoptosis in tumor cells by activation of death receptors 4/5. This phase 1 dose-escalation/dose-optimization study evaluated the safety, pharmacokinetics, pharmacodynamics, and preliminary activity of eftoza in patients with advanced solid tumors. Patients received eftoza 2.5–15 mg/kg intravenously on day 1 or day 1/day 8 every 21 days in the dose-escalation phase, and 1.25–7.5 mg/kg once-weekly (QW) in the dose-optimization phase. Dose-limiting toxicities (DLTs) were evaluated during the first treatment cycle to determine the maximum tolerated dose (MTD) and recommended phase 2 dose (RP2D). Pharmacodynamic effects were evaluated in circulation and tumor tissue. A total of 105 patients were enrolled in the study (dose-escalation cohort, n = 57; dose-optimization cohort, n = 48 patients [n = 24, colorectal cancer (CRC); n = 24, pancreatic cancer (PaCA)]). In the dose-escalation cohort, seven patients experienced DLTs. MTD and RP2D were not determined. Most common treatment-related adverse events were increased alanine aminotransferase and aspartate aminotransferase levels, nausea, and fatigue. The one treatment-related death occurred due to respiratory failure. In the dose-optimization cohort, three patients (CRC, n = 2; PaCA, n = 1) had a partial response. Target engagement with regard to receptor saturation, and downstream apoptotic pathway activation in circulation and tumor were observed. Eftoza had acceptable safety, evidence of pharmacodynamic effects, and preliminary anticancer activity. The 7.5-mg/kg QW regimen was selected for future studies on the basis of safety findings, pharmacodynamic effects, and biomarker modulations. (Trial registration number: NCT03082209 (registered: March 17, 2017)).

Published

2022

29. Phase II trial of oral beta-all trans-retinoic acid in hepatocellular carcinoma (SWOG 9157).

Author

Meyskens, F L, Jr, Jacobson, J, Nguyen, B, Weiss, G R, Gandara, D R, and MacDonald, J S

Subjects

Administration, Oral, Carcinoma, Hepatocellular: drug therapy, Humans, Liver Neoplasms: drug therapy, Survival Rate, Tretinoin: adverse effects, therapeutic use, Hepatocellular carcinoma, Hepatoma, Retinoic acid, Vitamin Abilirubin, creatinine, retinoic acid, anemia, antineoplastic activity, arthralgia, article, bilirubin blood level, cancer survival, clinical article, clinical trial, creatinine blood level, diarrhea, drug efficacy, dry skin, fatigue, headache, human, hypercalcemia, lethargy, liver cell carcinoma, liver function test, malaise, myalgia, nausea, oral drug administration, phase 2 clinical trial, priority journal, stomatitis, survival time, vomiting, Administration, Oral, Carcinoma, Hepatocellular, Humans, Liver Neoplasms, Survival Rate, Tretinoin

Abstract

Twenty-nine chemotherapy-naive patients with primary hepatocellular carcinoma were treated with oral beta-all trans-retinoic acid (retinoic acid, TRA 50 mg/m2 t.i.d.) on a 3-week on/one week off schedule until progression or grade 3 or 4 toxicity. Eligibility requirements allowed abnormal liver function tests as long as the creatinine and bilirubin levels were normal. No responses were seen and the median survival was four months. Grade 3 side effects occurred in II patients and grade 4 in four and included a wide range of toxicities. The results indicate that oral TRA is ineffective against primary hepatocellular carcinoma and suggest that dose-modification of this retinoid may be required in patients with significant malignant hepatic involvement.

Published

1998

30. A phase 1 study to assess the safety, pharmacokinetics, and anti-tumor activity of the androgen receptor n-terminal domain inhibitor epi-506 in patients with metastatic castration-resistant prostate cancer

Author

Leah DiMascio, Frank Perabo, Corinne Maurice-Dror, Ronan Le Moigne, Michael S. Gordon, Ulka N. Vaishampayan, Kim N. Chi, Nan Hyung Hong, and Robert B. Montgomery

Subjects

Pharmacology, Oncology, medicine.medical_specialty, business.industry, Nausea, medicine.disease, Androgen receptor, Prostate cancer, Pharmacokinetics, Tolerability, Internal medicine, Vomiting, Medicine, Potency, Pharmacology (medical), medicine.symptom, business, Adverse effect

Abstract

BACKGROUND EPI-506 is the first of a new class of drugs targeting the N-terminal domain (NTD) of the androgen receptor (AR), potentially overcoming known resistance mechanisms to androgen receptor pathway inhibitors (ARPIs) among men with metastatic castration resistant prostate cancer (mCRPC). METHODS Patients with mCRPC who had progressed on prior ARPI were enrolled in this phase 1 open-label, adaptive 3 + 3 dose escalation study. The primary outcome was safety and tolerability of oral EPI-506. Secondary objectives included determination of the maximal tolerated dose (MTD), pharmacokinetic profile, and antitumor efficacy. RESULTS 28 mCRPC patients were enrolled into 7 dose cohorts of EPI-506 ranging from 80-3600 mg given once daily and 1800 mg given twice daily. Six DLTs occurred in 4 patients; Grade 4 elevated amylase; Grade 3 abdominal pain; Grade 3 elevated ALT and Grade 3 elevated AST; Grade 2 nausea and Grade 1 vomiting which resulted in study drug intake of

Published

2021

31. A phase i study of ixazomib and erlotinib in patients with advanced solid tumors

Author

Mianen Sun, Ly M. Nguyen, Elsa J. Brown, David S. Hong, Shumei Kato, Siqing Fu, Timothy A. Yap, Sarina Anne Piha-Paul, Vivek Subbiah, Daniel D. Karp, and Jacob J. Adashek

Subjects

Pharmacology, Oncology, medicine.medical_specialty, business.industry, Nausea, medicine.disease, Rash, Ixazomib, chemistry.chemical_compound, chemistry, Internal medicine, medicine, Proteasome inhibitor, Pharmacology (medical), Sarcoma, Erlotinib, medicine.symptom, business, Adverse effect, medicine.drug, EGFR inhibitors

Abstract

Background. Preclinical studies have shown that the combined inhibition of EGFR and NF-kB pathways to target the RalB/TBK1 pathway led to synergistic antitumor activity. Based on this rationale, we conducted a Phase I dose-escalation study combining the EGFR inhibitor erlotinib with the NF-kB inhibitor ixazomib in advanced solid tumors. Patients and methods. Patients with advanced solid tumors were eligible. The bayesian optimal interval phase I dose escalation design was used to establish the maximum tolerated dose and recommended phase 2 dose (RP2D). Results. Nineteen patients with a range of solid tumors were enrolled. The most common treatment-related adverse events of any grade were diarrhea (42.1%, 8/19), followed by rash (36.8%, 7/19) and nausea (21.1%, 4/19). The combination RP2D for oral ixazomib was 4.0 mg on days 1, 8, and 15 of a 28-day cycle, with oral erlotinib 150 mg daily. While no patient achieved RECIST v1.1 objective responses, 3 patients with advanced sarcoma experienced durable RECIST v1.1 stable disease ≥ 6 months (8.4, 10.6, and 15.7 months) and the best response was -13% decrease in clear cell sarcoma. Conclusions. The combination of erlotinib and ixazomib was safe and well tolerated among patients with advanced cancer, with preliminary signals of antitumor activity in patients with advanced sarcoma.

Published

2021

32. A phase I trial to determine safety and pharmacokinetics of ASLAN002, an oral MET superfamily kinase inhibitor, in patients with advanced or metastatic solid cancers.

Author

Roohullah, Aflah, Cooper, Adam, Lomax, Anna J., Aung, Jennifer, Barge, Alan, Chow, Lilian, McHale, Mark, Desai, Jayesh, Whittle, James R., Tran, Ben, de Souza, Paul, and Horvath, Lisa G.

Subjects

ATRIAL fibrillation, CLINICAL trials, CONSTIPATION, DOSE-effect relationship in pharmacology, FATIGUE (Physiology), METASTASIS, NAUSEA, ORAL drug administration, TUMORS, TUMOR classification, PROTEIN-tyrosine kinase inhibitors, TREATMENT effectiveness, DISEASE incidence, THERAPEUTICS

Abstract

Background The MET tyrosine kinase and its ligand, hepatocyte growth factor (HGF) also known as scatter factor, are associated with tumourigenesis and metastasis by promotion of scattering, proliferation, angiogenesis, motility and invasion. ASLAN-002 is a potent inhibitor of MET as well as related kinases. A phase I dose escalation study was conducted to determine the safety and pharmacokinetics of ASLAN-002 in patients with advanced cancer. Methods Patients with advanced or metastatic solid tumours, who had progressed on standard therapy or for whom standard therapy was not known, were administered ASLAN-002 orally. The starting dose was 100 mg once daily (QD) with subsequent cohorts to receive doses of 200 mg QD, 300 mg QD, 450 mg QD, 600 mg QD, 300 mg twice daily (BID), 450 mg BID, and 600 mg BID. Results Forty patients were included across 7 dose cohorts. Cohort 8 (600 mg BID) was not opened due to the lack of appreciable pharmacokinetic (PK) differences between 300 mg BID and 450 mg BID and higher incidences of grade 3 or 4 adverse events (AE) in Cohort 7 (450 mg BID). Fifteen patients (37.5%) experienced a grade 3 or 4 AE. The most commonly reported AEs were nausea (55%), fatigue (47.5%) and constipation (30%). One dose limiting toxicity (DLT) of atrial fibrillation was observed with 450 mg BID. Conclusions ASLAN-002 is well tolerated at 300 mg BID and is the recommended dose for future phase II studies (RP2D). Clinical Trials Registry Number: NCT01721148. [ABSTRACT FROM AUTHOR]

Published

2018

33. A phase 1 study of PARP-inhibitor ABT-767 in advanced solid tumors with BRCA1/2 mutations and high-grade serous ovarian, fallopian tube, or primary peritoneal cancer.

Author

van der Biessen, Diane A. J., Gietema, Jourik A., de Jonge, Maja J. A., Desar, Ingrid M. E., den Hollander, Martha W., Dudley, Matthew, Dunbar, Martin, Hetman, Robert, Serpenti, Camille, Xiong, Hao, Mittapalli, Rajendar K., Timms, Kirsten M., Ansell, Peter, Ratajczak, Christine K., Shepherd, Stacie Peacock, and van Herpen, Carla M. L.

Subjects

ANEMIA, BIOAVAILABILITY, CLINICAL trials, DOSE-effect relationship in pharmacology, EATING disorders, ENZYME inhibitors, FALLOPIAN tubes, FATIGUE (Physiology), GENETIC mutation, NAUSEA, ORAL drug administration, SURVIVAL, TUMOR markers, OVARIAN tumors, TUMOR classification, PERITONEUM tumors, BRCA genes, DISEASE progression, DIAGNOSIS, PROGNOSIS, GENETICS

Abstract

Purpose This phase 1 study examined safety, pharmacokinetics (PK), and efficacy of the poly(ADP-ribose) polymerase (PARP) inhibitor ABT-767 in patients with advanced solid tumors and BRCA1/2 mutations or with high-grade serous ovarian, fallopian tube, or primary peritoneal cancer. Methods Patients received ABT-767 monotherapy orally until disease progression or unacceptable toxicity. Dose was escalated from 20 mg once daily to 500 mg twice daily (BID). Dose-limiting toxicities, recommended phase 2 dose (RP2D), food effect, objective response rate, and biomarkers predicting response were determined. Results Ninety-three patients were treated with ABT-767; 80 had a primary diagnosis of ovarian cancer. ABT-767 demonstrated dose-proportional PK up to 500 mg BID and half-life of ~2 h. Food had no effect on ABT-767 bioavailability. Most common grade 3/4 treatment-related adverse events were nausea, fatigue, decreased appetite, and anemia. Anemia showed dose-dependent increase. RP2D was 400 mg BID. Objective response rate by RECIST 1.1 was 21% (17/80) in all evaluable patients and 20% (14/71) in evaluable patients with ovarian cancer. Response rate by RECIST 1.1 and/or CA-125 was 30% (24/80) in patients with ovarian cancer. Mutations in BRCA1 or BRCA2, homologous recombination deficiency (HRD), and platinum sensitivity were associated with tumor response. Median progression-free survival was longer for HRD positive (6.7 months) versus HRD negative patients (1.8 months) with ovarian cancer. Conclusions ABT-767 had an acceptable safety profile up to the established RP2D of 400 mg BID and dose-proportional PK. Patients with BRCA1 or BRCA2 mutation, HRD positivity, and platinum sensitivity were more sensitive to ABT-767. [ABSTRACT FROM AUTHOR]

Published

2018

34. A multicentre, open-label phase II study of Irinotecan, capecitabine (Xeloda®), and Oxaliplatin (IXO) as first-line treatment in patients with metastatic gastric or gastroesophageal junction (GEJ) adenocarcinoma.

Author

Lui, Arthur, Mulder, Karen, Brezden-Masley, Christine, Vickers, Michael, Monzon, Jose, Kennecke, Hagen, Goel, Rakesh, Vos, Larissa, Ghosh, Sunita, Marginean, Horia, Fields, Anthony, Maroun, Jean, and Spratlin, Jennifer

Subjects

THERAPEUTIC use of antimetabolites, IRINOTECAN, ADENOCARCINOMA, CLINICAL trials, DIARRHEA, DOSE-effect relationship in pharmacology, DRUG side effects, DRUG toxicity, ESOPHAGUS, FATIGUE (Physiology), HYPOKALEMIA, INTRAVENOUS therapy, MEDICAL cooperation, METASTASIS, NAUSEA, NEUTROPENIA, ONCOGENES, RESEARCH, STOMACH tumors, SURVIVAL, OXALIPLATIN, TREATMENT effectiveness, PROGNOSIS, THERAPEUTICS

Abstract

Purpose Chemotherapy remains the primary treatment for metastatic gastric/GEJ cancer but optimal agents and schedule remain controversial. This study examined the safety and efficacy of first-line Irinotecan, capecitabine (Xeloda®), and Oxaliplatin (IXO). Patients and Methods Eligible patients with HER2-unamplified/unknown, metastatic gastric/GEJ adenocarcinoma were treated with 21-day cycle IXO at dose level 1 (DL1: Day 1 O-100 mg/m2 & I-160 mg/m2 IV, Day 2-15 X-1900 mg/m2/day PO divided doses) or modified IXO (mIXO): Day 1 O-85 mg/m2 & I-120 mg/m2 IV, Day 2-15 X-1425 mg/m2/day PO divided doses). This Bryant and Day two-stage designed study had dual primary endpoints of objective response rate (ORR) and toxicity. Secondary endpoints were overall survival (OS) and progression-free survival (PFS). Results Fifty patients were enrolled and received a median of 7 cycles. After accrual of 9 patients at DL1, evaluable RR was 88% however dose limiting toxicity (DLT) rate was 56% thus doses were adjusted to mIXO. Fifteen patients accrued at mIXO had a RR of 60% and DLT rate of 13% allowing continuation to stage 2. Overall, 48 and 49 patients were evaluable for efficacy and safety, respectively, with ORR of 54% and DLTs in 24% of patients (DL1 = 56%; mIXO = 18%). Disease control rate was 85%. The most frequent grade 3/4 adverse events were diarrhea, neutropenia, fatigue, hypokalemia, and nausea. Median PFS and OS were 7.5 and 13.0 months, respectively, with a median follow-up of 9.7 months. Conclusion mIXO demonstrates promising ORR, PFS, OS, and acceptable toxicity compared to standard triplet regimens. IXO should be evaluated in phase III trials. [ABSTRACT FROM AUTHOR]

Published

2018

35. A phase I and pharmacokinetic study of taladegib, a Smoothened inhibitor, in Japanese patients with advanced solid tumors.

Author

Ueno, Hideki, Kondo, Shunsuke, Yoshikawa, Shusuke, Inoue, Koichi, Andre, Valérie, Tajimi, Masaomi, and Murakami, Haruyasu

Subjects

ANTINEOPLASTIC agents, BASAL cell carcinoma, BODY weight, CLINICAL trials, DRUG tolerance, DOSE-effect relationship in pharmacology, DRUG side effects, DRUG toxicity, EATING disorders, FATIGUE (Physiology), GLIOMAS, GROWTH factors, NAUSEA, ONCOGENES, ORAL drug administration, PHARMACEUTICAL chemistry, TASTE disorders, THROMBOCYTOPENIA, TUMORS, TUMOR classification, VOMITING, TREATMENT effectiveness

Abstract

Background This phase I dose-escalation study investigated the safety of the Smoothened inhibitor taladegib in Japanese patients with advanced solid tumors. Methods Patients received taladegib orally once daily for 28-day cycles, using a 3 + 3 dose-escalation method. The primary objective was the safety and tolerability of taladegib at doses up to the global recommended dose (400 mg). Secondary objectives included pharmacokinetics, changes in skin glioma-associated oncogene homolog 1 (Gli1) transcript levels, and antitumor activity. Results Nineteen patients received treatment (100 mg: 3; 200 mg: 3; 400 mg: 13). No dose-limiting toxicities (DLTs) were observed at doses of 100 mg or 200 mg; 3 of the 9 patients evaluable for DLTs at the 400 mg dose level experienced DLTs (thrombocytopenia: 1; decreased appetite: 2). The most commonly reported treatment-related adverse events were dysgeusia (13/19, 68.4%), decreased appetite (12/19, 63.2%), nausea (9/19, 47.4%), fatigue (9/19, 47.4%), and vomiting (6/19, 31.6%). The pharmacokinetic profile suggested that exposure to taladegib was higher in Japanese than non-Japanese patients, possibly related to differences in body weight and/or drug formulation. At all dose levels, a high level of inhibition of skin Gli1 transcript levels was observed after 15 and 30 days of exposure to taladegib. Partial response was achieved by 1 patient (basal cell carcinoma of the skin) and stable disease by 4 patients. Conclusions Taladegib doses of 100 mg and 200 mg, but not the global recommended dose of 400 mg, were well tolerated in this population of Japanese patients with advanced solid tumors. [ABSTRACT FROM AUTHOR]

Published

2018

36. Phase1 study of cisplatin plus pemetrexed with erlotinib and bevacizumab for chemotherapy-naïve advanced non-squamous non-small cell lung cancer with EGFR mutations.

Author

Tamiya, Motohiro, Tamiya, Akihiro, Shiroyama, Takayuki, Takeoka, Sawa, Naito, Yujiro, Omachi, Naoki, Kimura, Yohei, Morishita, Naoko, Suzuki, Hidekazu, Okamoto, Norio, Okishio, Kyoichi, Kawaguchi, Tomoya, Atagi, Shinji, and Hirashima, Tomonori

Subjects

LUNG cancer & genetics, LUNG cancer prognosis, ANOREXIA nervosa, CANCER chemotherapy, COMBINATION drug therapy, CISPLATIN, CLINICAL trials, DRUG dosage, DOSE-effect relationship in pharmacology, DRUG side effects, DRUG toxicity, EPIDERMAL growth factor, EXANTHEMA, FATIGUE (Physiology), FEBRILE neutropenia, GASTROINTESTINAL hemorrhage, LUNG cancer, GENETIC mutation, NAUSEA, SURVIVAL, SQUAMOUS cell carcinoma, TREATMENT effectiveness, BEVACIZUMAB, ERLOTINIB, PEMETREXED, GENETICS, THERAPEUTICS, PROGNOSIS

Abstract

Background Cisplatin and pemetrexed are very effective against advanced non-squamous non-small cell lung cancer (NSCLC) without EGFR mutations. Erlotinib plus bevacizumab are highly effective against advanced NSCLCs with activating EGFR mutations. We performed this phase I ‘Quartet Trial’ to determine the safety and efficacy of all 4 agents as a first-line treatment for non-squamous NSCLC patients harboring activating EGFR mutations. Patients and Methods Patients received escalating quartet-agent doses every 3 weeks for 4 cycles. We examined the dose-limiting toxicity (DLT) to determine the maximum tolerated dose (MTD) and recommended dose (RD). Results Ten patients (3 men and 7 women) with a median age of 69 years were enrolled. Four and 6 patients had exon 19 and 21 mutations, respectively; 8 received maintenance therapy without unexpected or cumulative toxicities. One of 6 patients experienced grade 3 vagal reflex at 60 mg/m2 cisplatin plus 500 mg/m2 pemetrexed with 150 mg erlotinib and 15 mg/kg bevacizumab, which was designated the RD. Four patients experienced no DLT with 75 mg/m2 cisplatin plus 500 mg/m2 pemetrexed with 150 mg erlotinib and 15 mg/kg bevacizumab (designated the MTD); however, 3 underwent dose reduction due to severe toxicities (grade 3 gastrointestinal hemorrhage, skin rash, nausea, and febrile neutropenia) during induction chemotherapy. The most frequent DLT-phase adverse events were nausea, anorexia, and fatigue. The overall response rate was 100%. Furthermore, the progression-free and overall survival rates were 17.9 and 32.0 months, respectively. Conclusions This quartet chemotherapy regimen was tolerable and effective in our patient population (UMIN000012536). [ABSTRACT FROM AUTHOR]

Published

2018

37. Dual Src and EGFR inhibition in combination with gemcitabine in advanced pancreatic cancer: phase I results.

Author

Cardin, Dana B., Goff, Laura W., Chan, Emily, Whisenant, Jennifer G., Dan Ayers, G., Takebe, Naoko, Arlinghaus, Lori R., Yankeelov, Thomas E., Berlin, Jordan, and Merchant, Nipun

Subjects

THERAPEUTIC use of antimetabolites, ANEMIA, ANTIMETABOLITES, ASPARTATE aminotransferase, COMBINATION drug therapy, CLINICAL trials, DRUG tolerance, DRUG toxicity, FATIGUE (Physiology), LEUCOPENIA, NAUSEA, NEUTROPENIA, ORAL drug administration, PANCREATIC tumors, SURVIVAL, THROMBOCYTOPENIA, ALANINE aminotransferase, TREATMENT effectiveness, LYMPHOPENIA, DASATINIB, ERLOTINIB, THERAPEUTICS

Abstract

Pancreatic adenocarcinoma remains a major therapeutic challenge, as the poor (<8%) 5-year survival rate has not improved over the last three decades. Our previous preclinical data showed cooperative attenuation of pancreatic tumor growth when dasatinib (Src inhibitor) was added to erlotinib (EGFR inhibitor) and gemcitabine. Thus, this study was designed to determine the maximum-tolerated dose of the triplet combination. Standard 3 + 3 dose escalation was used, starting with daily oral doses of 70 mg dasatinib and 100 mg erlotinib with gemcitabine on days 1, 8, and 15 (800 mg/m2) of a 28-day cycle (L0). Nineteen patients were enrolled, yet 18 evaluable for dose-limiting toxicities (DLTs). One DLT observed at L0, however dasatinib was reduced to 50 mg (L−1) given side effects observed in the first two patients. At L−1, a DLT occurred in 1/6 patients and dose was re-escalated to L0, where zero DLTs reported in next four patients. Dasatinib was escalated to 100 mg (L1) where 1/6 patients experienced a DLT. Although L1 was tolerable, dose escalation was stopped as investigators felt L1 was within the optimal therapeutic window. Most frequent toxicities were anemia (89%), elevated aspartate aminotransferase (79%), fatigue (79%), nausea (79%), elevated alanine aminotransferase (74%), lymphopenia (74%), leukopenia (74%), neutropenia (63%), and thrombocytopenia (63%), most Grade 1/2. Stable disease as best response was observed in 69% (9/13). Median progression-free and overall survival was 3.6 and 8 months, respectively. Dasatinib, erlotinib, and gemcitabine was safe with manageable side effects, and with encouraging preliminary clinical activity in advanced pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2018

38. Safety, pharmacokinetic, and pharmacodynamics of erdafitinib, a pan-fibroblast growth factor receptor (FGFR) tyrosine kinase inhibitor, in patients with advanced or refractory solid tumors.

Author

Nishina, Tomohiro, Takahashi, Shunji, Iwasawa, Ryota, Noguchi, Hidehisa, Aoki, Masayuki, and Doi, Toshihiko

Subjects

TUMOR diagnosis, CELL lines, CELL receptors, CLINICAL trials, ELECTROCARDIOGRAPHY, NAUSEA, RETINAL detachment, STOMATITIS, TASTE disorders, TUMORS, PROTEIN-tyrosine kinase inhibitors, TREATMENT effectiveness, HYPERPHOSPHATEMIA, PHARMACODYNAMICS

Abstract

Introduction This phase 1, open-label, multicenter, single-arm, dose-escalation study aimed to evaluate safety, pharmacokinetics (PK), and pharmacodynamics of erdafitinib (JNJ-42756493), an oral selective pan-fibroblast growth factor receptor (FGFR) tyrosine kinase inhibitor, and to determine the recommended phase 2 dose in Japanese patients with advanced or refractory solid tumors. Methods Three to 6 patients were enrolled into sequentially escalating dose cohorts (erdafitinib 2, 4, or 6 mg) with a daily dosing schedule of 21-day cycles or a 7 days-on/7 days-off intermittent schedule (erdafitinib 10 mg or 12 mg) of 28-day cycles. Results Nineteen patients received escalating doses of erdafitinib with a daily or intermittent schedule. The most common treatment-emergent adverse events (TEAEs) were hyperphosphatemia (73.7%), nausea (36.8%), stomatitis (26.3%), dysgeusia (26.3%) and dry mouth (21.1%). The maximum tolerated dose was not reached in this study. No Grade 3 or higher TEAEs, or serious TEAEs were noted and no clinically significant changes in vital signs, laboratory parameters, and electrocardiogram readings were observed. However, one case of dose-limiting toxicity in the 12 mg intermittent dosing group was observed: Grade 2 detachment of retinal pigment epithelium (bilateral) with treatment discontinuation. The maximum plasma concentrations of erdafitinib exhibited a dose-dependent increase. The median tmax ranged from 2 to 3 h after the initial dose to 2-6 h following multiple daily dosing. Based on the safety and PK data, the 10 mg 7 days-on/7 days-off regimen was determined as the recommended phase 2 dose in this study. Conclusions Erdafitinib was well tolerated in Japanese patients with advanced or refractory solid tumors. Trial Registration: NCT01962532. [ABSTRACT FROM AUTHOR]

Published

2018

39. Safety, tolerability, and pharmacokinetic profile of dabrafenib in Japanese patients with BRAFV600 mutation-positive solid tumors: a phase 1 study.

Author

Yutaka Fujiwara, Naoya Yamazaki, Yoshio Kiyohara, Shusuke Yoshikawa, Noboru Yamamoto, Arata Tsutsumida, Hiroshi Nokihara, Kenjiro Namikawa, Akihira Mukaiyama, Fanghong Zhang, and Tomohide Tamura

Subjects

ANTINEOPLASTIC agents, BALDNESS, CLINICAL trials, DRUG tolerance, LEUCOPENIA, MELANOMA, GENETIC mutation, NAUSEA, ONCOGENES, PATIENT safety, PROTEIN kinases, THYROID gland tumors, TUMORS, TREATMENT effectiveness, JOINT pain

Abstract

Background Dabrafenib is a BRAF inhibitor that has demonstrated clinical activity with a good tolerability profile in patients with BRAFV600E mutated metastatic melanoma. This study evaluated the safety and tolerability, pharmacokinetics and preliminary efficacy of dabrafenib in Japanese patients. Methods This phase I, open-label, dose escalation study was conducted in 12 Japanese patients with BRAFV600 mutation positive solid tumours. Primary endpoint was safety, assessed by monitoring and recording of all adverse events (AEs), serious AEs, drug-related AEs; secondary endpoints were pharmacokinetic profiles and efficacymeasured by tumour response. This study is registered with ClinicalTrials.gov, number NCT01582997. Results Of the 12 patients enrolled, 3 each received 75mg and 100 mg dabrafenib while 6 received 150 mg dabrafenib twice daily orally. Melanoma and thyroid cancer were the primary tumours reported in 11 (92%) and 1 (8%) patients respectively. Most AEs were grade 1 or 2 and considered related to study treatment. Most common AEs reported in the 12 patients were alopecia in 7 (58%); pyrexia, arthralgia and leukopenia in 6 (50%) each, hyperkeratosis and nausea in 4 (33%) each. Partial response as best overall response was reported in 7 of 12 (58%) patients and in 6 (55%) with malignant melanoma. No dose-limiting toxicity (DLTs) were reported during the DLT evaluation periods. Conclusions Dabrafenib was well tolerated and rapidly absorbed administered as single- or multiple dose. Comparable safety and pharmacokinetic profiles were observed compared with non-Japanese patients. Dabrafenib has promising clinical activity in Japanese patients with BRAF mutated malignant melanoma. [ABSTRACT FROM AUTHOR]

Published

2018

40. A phase 2 study of ontuxizumab, a monoclonal antibody targeting endosialin, in metastatic melanoma.

Author

D’Angelo, Sandra P., Hamid, Omid A., Tarhini, Ahmad, Schadendorf, Dirk, Chmielowski, Bartosz, Collichio, Frances A., Pavlick, Anna C., Lewis, Karl D., Weil, Susan C., Heyburn, John, Schweizer, Charles, O’Shannessy, Daniel J., and Carvajal, Richard D.

Subjects

THERAPEUTIC use of monoclonal antibodies, BIOMARKERS, CONFIDENCE intervals, CLINICAL drug trials, FATIGUE (Physiology), HEADACHE, MELANOMA, METASTASIS, MONOCLONAL antibodies, NAUSEA, NEOVASCULARIZATION, DISEASE progression, DESCRIPTIVE statistics

Abstract

Objectives Ontuxizumab (MORAB-004) is a first-in-class monoclonal antibody that interferes with endosialin function, which is important in tumor stromal cell function, angiogenesis, and tumor growth. This Phase 2 study evaluated the 24-week progression-free survival (PFS) value, pharmacokinetics, and tolerability of 2 doses of ontuxizumab in patients with metastatic melanoma. Patients and methods Patients with metastatic melanoma and disease progression after receiving at least 1 prior systemic treatment were randomized to receive ontuxizumab (2 or 4 mg/kg) weekly, without dose change, until disease progression. Results Seventy-six patients received at least 1 dose of ontuxizumab (40 received 2 mg/kg, 36 received 4 mg/kg). The primary endpoint, 24-week PFS value, was 11.4% (95% Confidence Interval [CI]: 5.3%–19.9%) for all patients (13.5% for 2 mg/kg and 8.9% for 4 mg/kg). The median PFS for all patients was 8.3 weeks (95% CI: 8.1–12.3 weeks). One patient receiving 4 mg/kg had a partial response, as measured by Response Evaluation Criteria in Solid Tumors v1.1. Twenty-seven of 66 response evaluable patients (40.9%) had stable disease. The median overall survival was 31.0 weeks (95% CI: 28.3–44.0 weeks). The most common adverse events overall were headache (55.3%), fatigue (48.7%), chills (42.1%), and nausea (36.8%), mostly grade 1 or 2. Conclusions Ontuxizumab at both doses was well tolerated. The 24-week PFS value was 11.4% among all ontuxizumab-treated patients. The overall response rate was 3.1% at the 4 mg/kg dose, with clinical benefit achieved in 42.4% of response evaluable patients. Efficacy of single-agent ontuxizumab at these doses in melanoma was low. [ABSTRACT FROM AUTHOR]

Published

2018

41. Metformin as a repurposed therapy in advanced non-small cell lung cancer (NSCLC): results of a phase II trial.

Author

Parikh, Anish, Kozuch, Peter, Rohs, Nicholas, Becker, Daniel, and Levy, Benjamin

Subjects

ANEMIA, ANTINEOPLASTIC agents, CANCER chemotherapy, CLINICAL trials, COMBINED modality therapy, DRUG side effects, CLINICAL drug trials, FATIGUE (Physiology), INSULIN, LONGITUDINAL method, LUNG cancer, GENETIC mutation, NAUSEA, SURVIVAL, METFORMIN, TREATMENT duration, DESCRIPTIVE statistics, CARBOPLATIN, PEMETREXED

Abstract

Background Metformin has been shown to have anti-neoplastic activity in non-small cell lung cancer (NSCLC) in both preclinical and observational studies, however this has never been prospectively evaluated. This single-arm phase II trial, while not fully accrued, is the first known prospective study evaluating the use of metformin with chemotherapy in advanced NSCLC. Methods Patients received carboplatin AUC 5 + pemetrexed 500 mg/m2 IV every 21 days for 4 cycles. For patients who achieved at least stable disease, maintenance pemetrexed was administered until progression or toxicity. Metformin was initiated at 1000 mg/day for week 1, 1500 mg/day for week 2, then 2000 mg/day thereafter, in divided doses. The primary endpoint was progression-free survival (PFS). Secondary endpoints were overall survival (OS), objective response rate (ORR), disease control rate (DCR), duration of response (DOR), and adverse events (AE). Tumor tissue was tested for LKB1/STK11 mutations, and non-fasting serum insulin levels were longitudinally assessed. Results Of a planned 50 patients, 14 were enrolled. ORR was 23% and median PFS was 3.9 months. Median OS was 11.7 months. No LKB1/STK11 mutations were identified. The most common AE were fatigue (42.9%), anemia, and nausea (28.6% each). The most common grade III AE was nausea (14.3%). No grade IV AE occurred. Mean duration of metformin treatment was 5.6 months. Conclusion Adding metformin to chemotherapy for advanced NSCLC was safe but did not significantly improve clinical outcomes compared to historical phase III controls. These results are limited by the small sample size; larger trials are needed. [ABSTRACT FROM AUTHOR]

Published

2017

42. A multicenter phase 1/2 study investigating the safety, pharmacokinetics, pharmacodynamics and efficacy of a small molecule antimetabolite, RX-3117, plus nab-paclitaxel in pancreatic adenocarcinoma

Author

Nafisa Burhani, Hani M. Babiker, Emad Elquza, Andrea J. Bullock, Ely Benaim, Allyson J. Ocean, Lee G. Hicks, Peter J. Schlegel, Christine B. Peterson, Daruka Mahadevan, Mitesh J. Borad, and Callie Heaton

Subjects

Pharmacology, medicine.medical_specialty, business.industry, Nausea, medicine.drug_class, medicine.disease, Gastroenterology, Antimetabolite, Gemcitabine, Oncology, Tolerability, Pharmacokinetics, Pancreatic cancer, Pharmacodynamics, Internal medicine, Medicine, Pharmacology (medical), medicine.symptom, Adverse effect, business, medicine.drug

Abstract

Background RX-3117 is an oral small molecule antimetabolite, cyclopentyl pyrimidyl nucleoside that is activated by cancer cells over-expressing uridine cytidine kinase 2 (UCK2). Single agent RX-3117 demonstrated efficacy in a phase I trial in patients with metastatic (met) pancreatic adenocarcinoma (PC). RX-3117 plus nab-paclitaxel (nab-Pac) was evaluated as a first line treatment in met-PC cancer. Methods This was a multicenter open label phase I/II 2-stage study investigating the combination of RX3117 plus nab-Pac in the frontline treatment of patients with met-PC. The phase I portion comprised a dose de-escalation design with primary objectives of determining the safety, tolerability and recommended phase 2 dose (RP2D) of RX-3117 (orally 700, 600, or 500 mg/day for 5 consecutive days with 2 days off/week) plus nab-Pac (intravenous (IV) 125 mg/m2 once weekly) for 3 weeks with 1 week off per a 4-week cycle. The primary objective was to determine the antitumor efficacy. Results 46 patients were enrolled (22 male/24 female; median age 67; 91% Caucasian). The RP2D of RX-3117 plus nab-Pac was 700 mg/day. No dose-limiting toxicities were observed (DLTs). The overall response rate (ORR) was 23.1% and disease control rate (DCR) 74.4%. RX-3117 pharmacokinetics (PK) results were similar to previously reported monotherapy phase 1 trial. All patients experienced a treatment emergent adverse event (TEAE) with the most common diarrhea, nausea, and fatigue.10.9% of patients experienced a serious adverse event (SAE) related to the combination. Conclusion RX-3117 plus nab-Pac in newly diagnosed met-PC patients demonstrated tolerability, safety, and early treatment efficacy.

Published

2021

43. Selinexor in combination with topotecan in patients with advanced or metastatic solid tumors: Results of an open-label, single-center, multi‐arm phase Ib study

Author

Filip Janku, Vivek Subbiah, Denái R. Milton, Deby C. Ogbonna, Abdulrazzak Zarifa, Shubham Pant, Kyaw Zin Thein, Rivka R. Colen, Sarina Anne Piha-Paul, Stacie Bean, Jing Gong, Jatin P. Shah, Apostolia Maria Tsimberidou, Aung Naing, Brett W. Carter, Lacey McQuinn, Daniel D. Karp, and Funda Meric-Bernstam

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Maximum Tolerated Dose, Nausea, medicine.medical_treatment, Active Transport, Cell Nucleus, Receptors, Cytoplasmic and Nuclear, Selinexor, Selective inhibitor of nuclear export (SINE), Karyopherins, Neutropenia, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Phase I Studies, Neoplasms, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Pharmacology (medical), Adverse effect, Aged, Pharmacology, Chemotherapy, Dose-Response Relationship, Drug, business.industry, Endometrial cancer, Cancer, Middle Aged, Triazoles, medicine.disease, KPT 330, Hydrazines, 030104 developmental biology, Oncology, Metastatic solid tumors, 030220 oncology & carcinogenesis, Vomiting, Female, Topotecan, medicine.symptom, business, medicine.drug

Abstract

SummaryBackground Selinexor, a first-in-class, oral selective inhibitor of nuclear export (SINE) compound inhibits Exportin-1(XPO1), had demonstrated synergistic activity with many chemotherapies and conferred in vivo antitumor efficacy in hematologic as well as solid tumors. Methods This open-label, single-center, multi-arm phase 1b study used a standard 3 + 3 design and a “basket type” expansion. Selinexor with intravenous topotecan was given in one of the 13 parallel arms. Patients with advanced or metastatic relapsed/refractory solid tumors following prior systemic therapy, or in whom the addition of selinexor to standard chemotherapy deemed appropriate, were eligible. Results Fourteen patients with the median age of 61 years (range, 22–68years) were treated, and the most common cancer types were gynecological cancers; ovarian (n = 5), endometrial (n = 2), and 1 each with fallopian tube and vaginal cancers. Of the 14 patients treated, 12 (86 %) had at least one treatment-related adverse event (TRAE). The most common TRAEs were anemia (71 %), thrombocytopenia (57 %), hyponatremia (57 %), vomiting (57 %), fatigue (50 %), nausea (50 %), and neutropenia (36 %). Two patients had dose limiting toxicities. One patient dosed at selinexor 80 mg had grade 3 nausea and vomiting and one patient dosed at selinexor 60 mg experienced grade 4 neutropenia and thrombocytopenia. Of the 13 efficacy evaluable patients, one (8 %) with endometrial cancer achieved unconfirmed partial response (uPR) and the time-to-treatment failure (TTF) was 48 weeks, whereas 6 of the 13 (46 %) patients had stable disease (SD) contributing to the clinical benefit rate of 46 %. The median TTF for all patients was 9 weeks (range, 2–48weeks). Conclusions Once weekly selinexor in combination with topotecan was viable and showed some preliminary tumor efficacy. The recommend phase 2 dose of selinexor was 60 mg once weekly in combination with IV topotecan.Trial registration: NCT02419495. Registered 14 April 2015, https://clinicaltrials.gov/ct2/show/NCT02419495

Published

2021

44. A phase 1b study of the Notch inhibitor crenigacestat (LY3039478) in combination with other anticancer target agents (taladegib, LY3023414, or abemaciclib) in patients with advanced or metastatic solid tumors

Author

Philippe A. Cassier, Gerard J. Oakley, Christophe Massard, Danni Yu, Bailey Anderson, Shubham Pant, William D. Tap, Analia Azaro, Jaime R. Merchan, Eunice Yuen, Antoine Italiano, and Karim A. Benhadji

Subjects

0301 basic medicine, Oncology, medicine.medical_specialty, Nausea, Notch signaling pathway, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Internal medicine, Medicine, Pharmacology (medical), Adverse effect, Abemaciclib, Mechanistic target of rapamycin, Tissue homeostasis, Pharmacology, biology, business.industry, Cancer, medicine.disease, 030104 developmental biology, chemistry, Tolerability, 030220 oncology & carcinogenesis, biology.protein, medicine.symptom, business

Abstract

Notch signaling plays an important role in development and tissue homeostasis. Deregulation of Notch signaling has been implicated in multiple malignancies. Crenigacestat (LY3039478), a potent Notch inhibitor, decreases Notch signaling and its downstream biologic effects. I6F-MC-JJCD was a multicenter, nonrandomized, open-label, Phase 1b study with 5 separate, parallel dose-escalations in patients with advanced or metastatic cancer from a variety of solid tumors, followed by a dose-confirmation phase in prespecified tumor types. This manuscript reports on 3 of 5 groups. The primary objective was to determine the recommended Phase 2 dose of crenigacestat in combination with other anticancer agents (taladegib, LY3023414 [dual inhibitor of phosphoinositide 3-kinase; mechanistic target of rapamycin], or abemaciclib). Secondary objectives included evaluation of safety, tolerability, efficacy, and pharmacokinetics. Patients (N = 63) received treatment between November 2016 and July 2019. Dose-limiting toxicities occurred in 12 patients, mostly gastrointestinal (diarrhea, nausea, vomiting). The maximum-tolerated dose of crenigacestat was 25 mg in Part B (LY3023414), 50 mg in Part C (abemaciclib), and not established in Part A (taladegib) due to toxicities. Patients had at least 1 adverse event (AE) and 75.0–82.6% were ≥ Grade 3 all-causality AEs. No patient had complete or partial response. Disease control rates were 18.8% (Part B) and 26.1% (Part C). The study was terminated before dose confirmation cohorts were triggered. This study demonstrated that crenigacestat combined with different anticancer agents (taladegib, LY3023414, or abemaciclib) was poorly tolerated, leading to lowered dosing and disappointing clinical activity in patients with advanced or metastatic solid tumors. NCT02784795 and date of registration: May 27, 2016.

Published

2021

45. Phase I first-in-human study of HLX07, a novel and improved recombinant anti-EGFR humanized monoclonal antibody, in patients with advanced solid cancers

Author

Xiaodi Zhang, Yunting Zhu, Ching-Liang Ho, Hsuan-Yu Lin, and Ming-Mo Hou

Subjects

0301 basic medicine, Monoclonal antibody, Adult, Male, medicine.medical_specialty, Efficacy, Maximum Tolerated Dose, Nausea, Taiwan, Antineoplastic Agents, Antibodies, Monoclonal, Humanized, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Internal medicine, Phase I Studies, Neoplasms, Solid tumors, medicine, Clinical endpoint, Humans, Pharmacology (medical), Prospective Studies, Adverse effect, Aged, Pharmacology, Aged, 80 and over, Toxicity, Dose-Response Relationship, Drug, business.industry, Middle Aged, Clinical trial, ErbB Receptors, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cohort, Vomiting, Female, medicine.symptom, business

Abstract

SummaryPurpose This study aimed to evaluate the safety and pharmacokinetic (PK) profiles of HLX07, a novel, recombinant, humanized anti-epidermal growth factor receptor (EGFR) antibody, in patients with advanced solid cancers who had failed standard therapy or for whom no standard therapy was available. Methods In this prospective, open-label, Phase I dose escalation study, patients aged ≥18 years (≥20 years for patients in Taiwan) with histologically-confirmed metastatic or recurrent epithelial carcinoma that had no K-RAS or B-RAF mutations were enrolled in a ‘3 + 3’ escalation design. HLX07 was administered weekly by 2-h intravenous infusion at doses ranging from 50 to 800 mg. The primary endpoint was summary listing of participants reporting treatment-emergent adverse events (TEAEs). Secondary endpoints included PK analysis, serum anti-HLX07 antibody assessments and efficacy. Results In total, 19 patients were enrolled between 1 October 2016 and 16 July 2019 to receive HLX07 at doses of 50 (n = 3), 100 (n = 3), 200 (n = 3), 400 (n = 3), 600 (n = 3) and 800 (n = 4) mg per week. All patients experienced at least one TEAE, most commonly fatigue (68.4%), nausea (47.4%), paronychia (31.6%) and vomiting (31.6%). Serious TEAEs were reported in 11 patients but only one serious TEAE (dyspnea in 600 mg cohort) was regarded as possibly related to study treatment. No dose limiting toxicity (DLT) was reported. Systemic exposure to HLX07 increased proportionally with dose. Anti-HLX07 antibodies were not detected in any patients. Conclusion HLX07 was well tolerated (at dose levels up to 800 mg/week) and promising in patients with advanced solid cancers.Clinical Trial Registration: The study was registered at ClinicalTrials.gov: NCT02648490 (Jan 7, 2016).

Published

2021

46. Phase 1 cohort expansion study of LY3023414, a dual PI3K/mTOR inhibitor, in patients with advanced mesothelioma

Author

Todd M. Bauer, Volker Wacheck, Evan W. Alley, Suhyun Kang, Sophie Callies, Anna M. Szpurka, Johanna C. Bendell, Melinda D. Willard, Anna M. Varghese, Marjorie G Zauderer, and Enrica Capelletto

Subjects

0301 basic medicine, Mesothelioma, Male, medicine.medical_specialty, Nausea, Pyridines, Antineoplastic Agents, Quinolones, Gastroenterology, LY3023414, Cohort Studies, 03 medical and health sciences, 0302 clinical medicine, Refractory, Internal medicine, Phase I Studies, medicine, Humans, Pharmacology (medical), Adverse effect, Aged, Phosphoinositide-3 Kinase Inhibitors, Pharmacology, Aged, 80 and over, Solid tumor, Dose-Response Relationship, Drug, business.industry, TOR Serine-Threonine Kinases, PI3K/mTOR inhibitor, Middle Aged, medicine.disease, 030104 developmental biology, Treatment Outcome, Oncology, Tolerability, 030220 oncology & carcinogenesis, Cohort, Vomiting, Peritoneal mesothelioma, Female, medicine.symptom, business

Abstract

SummaryBACKGROUND LY3023414 is a selective, ATP competitive inhibitor of class I PI3K isoforms, mTORC1/2 and DNA-PK. A Phase 1 dose escalation, 200 mg twice daily (BID) of LY3023414 was the determined recommended phase 2 dose (RP2D). We report the antitumor activity and safety of LY3023414 monotherapy in patients with advanced mesothelioma.METHODS Patients enrolled had advanced malignant pleural or peritoneal mesothelioma with measurable disease, ECOG PS 0–1, were refractory or ineligible to receive standard therapies. Patients received LY3023414 200 mg BID. This dose expansion cohort is intended to evaluate preliminary antitumor activity of LY3023414 by overall response rate. Safety, tolerability and pharmacokinetics were assessed. Biomarkers associated with treatment response was an exploratory endpoint. RESULTS Forty-two patients received LY3023414 for a median duration of 11.2 weeks (range: 1.1–53.0). One patient had a confirmed partial response (PR) (ORR 2.4%). Three patients had an unconfirmed PR. Seventeen patients had stable disease (SD) (DCR 43%). Most common adverse events (AEs) included fatigue (43%), nausea (43%), decreased appetite (38%), vomiting (33%), and diarrhea (29%). AEs were mostly mild or moderate. Grade ≥ 3 AEs were reported for 21% of patients with fatigue as the most frequent event (10%). Alterations of BAP1 were identified in 11/19 patients as the most common molecular aberration, followed by SETD2 and NF2 alterations. No obvious pattern of genetic changes/mutations in single genes or pathways was associated with anti-tumor activity. CONCLUSION LY3023414 monotherapy (200 mg BID) demonstrated an acceptable and manageable safety profile with limited single-agent activity in patients with advanced mesothelioma. ClinicalTrials.gov identifier: NCT01655225; Date of registration: 19 July 2012.

Published

2021

47. LY3022855, an anti–colony stimulating factor-1 receptor (CSF-1R) monoclonal antibody, in patients with advanced solid tumors refractory to standard therapy: phase 1 dose-escalation trial

Author

Sonya C. Chapman, Michelle Carlsen, Robert Wesolowski, Omid Hamid, Richard D. Carvajal, R. Donald Harvey, Daniel A. Peterson, Afshin Dowlati, Anna M. Szpurka, Danni Yu, John S. Kauh, Samuel J. Klempner, and Tonya Quinlan

Subjects

0301 basic medicine, medicine.medical_specialty, Nausea, Population, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Internal medicine, Medicine, Pharmacology (medical), education, Adverse effect, Pharmacology, education.field_of_study, business.industry, medicine.disease, 030104 developmental biology, Oncology, Tolerability, 030220 oncology & carcinogenesis, Vomiting, Pancreatitis, Liver function, medicine.symptom, business

Abstract

Background Tumor-associated macrophages (TAMs) promote tumor growth, metastasis, and therapeutic resistance via colony-stimulating factor-1 (CSF-1), acting through CSF-1 receptor (CSF-1R) signaling. This phase 1 study determined the safety, tolerability, pharmacokinetics-pharmacodynamics, immunogenicity, and efficacy of the anti–CSF-1R antibody LY3022855 in solid tumors. Methods Patients with advanced solid tumors refractory to standard therapy were enrolled and treated in 2 dosing cohorts: weight-based (part A) and non–weight-based (part B). Part A patients were assigned to intravenous (IV) dose-escalation cohorts: 2.5 mg/kg once per week (QW), 0.3 mg/kg QW, 0.6 mg/kg QW, 1.25 mg/kg once every 2 weeks (Q2W) and 1.25 mg/kg QW doses of LY3022855. Non–weight-based doses in part B were 100 mg and 150 mg IV QW. Results Fifty-two patients (mean age 58.6 ± 10.4 years) were treated with ≥1 dose of LY3022855 (range: 4–6). Five dose-limiting toxicities (left ventricular dysfunction, anemia, pancreatitis, rhabdomyolysis, and acute kidney injury) occurred in 4 patients. The non–weight-based 100 mg QW dose was established as the RP2D. The most common treatment-emergent adverse events were increase in liver function variables, fatigue, nausea, vomiting, diarrhea, anorexia, pyrexia, increased lipase, amylase, and lactate dehydrogenase. Clearance decreased with increasing dose and weight-based dosing had minimal effect on pharmacokinetics. Serum CSF-1, and IL-34 levels increased at higher doses and more frequent dosing, whereas TAMs and CD14dimCD16bright levels decreased. Three patients achieved stable disease. No responses were seen. Conclusions LY3022855 was well tolerated and showed dose-dependent pharmacokinetics-pharmacodynamics and limited clinical activity in a heterogenous solid tumor population. ClinicalTrials.gov ID NCT01346358 (Registration Date: May 3, 2011).

Published

2021

48. Aurora kinase A inhibitor, LY3295668 erbumine: a phase 1 monotherapy safety study in patients with locally advanced or metastatic solid tumors

Author

Amparo de la Peña, Yu-Hua Hui, Patricia S Smith, Quincy Siu-Chung Chu, John R. Stille, Jill D. Kremer, Caroline Fortier, Gerald Batist, Eunice Yuen, Sara L. Zaknoen, Andrew Lithio, and Nathaniel Bouganim

Subjects

Adult, Male, 0301 basic medicine, Oncology, medicine.medical_specialty, Constipation, Maximum Tolerated Dose, Nausea, Aurora A kinase, 03 medical and health sciences, 0302 clinical medicine, Piperidines, Neoplasms, Internal medicine, Mucositis, Humans, Medicine, Pharmacology (medical), Adverse effect, Protein Kinase Inhibitors, Aged, Aurora Kinase A, Pharmacology, Dose-Response Relationship, Drug, business.industry, Cancer, Middle Aged, medicine.disease, Diarrhea, Treatment Outcome, 030104 developmental biology, Tolerability, 030220 oncology & carcinogenesis, Pyrazoles, Female, medicine.symptom, business

Abstract

Background Aurora A kinase (AurA) overexpression likely contributes to tumorigenesis and therefore represents an attractive target for cancer therapeutics. This phase 1 study aimed to determine the safety, pharmacokinetics, and antitumor activity of LY3295668 erbumine, an AurA inhibitor, in patients with locally advanced or metastatic solid tumors. Methods Patients with locally advanced or metastatic solid tumors, Eastern Cooperative Oncology Group performance status 0–1, and disease progression after one to four prior treatment regimens were enrolled. Primary objective was to determine maximum tolerated dose (MTD); secondary objectives included evaluation of the tolerability and safety profile and pharmacokinetics of LY3295668. All patients received twice-daily (BID) oral LY3295668 in 21-day cycles in an ascending-dose schedule. Results Twelve patients were enrolled in phase 1 (25 mg, n = 8; 50 mg, n = 2; 75 mg, n = 2) and one patient was enrolled after. Overall, four patients experienced dose-limiting toxicities (DLTs) within the first cycle (75 mg: Grade 3 diarrhea [one patient], Grade 4 mucositis and Grade 3 corneal deposits [one patient]; 50 mg: mucositis and diarrhea [both Grade 3, one patient]; 25 mg: Grade 3 mucositis [one patient]). Patients exhibiting DLTs had the highest model-predicted exposures at steady state. Mucositis was the most common adverse event (67%), followed by diarrhea, fatigue, alopecia, anorexia, constipation, and nausea. Nine patients had best response of stable disease; the disease control rate was 69%. Conclusions MTD of LY3295668 was 25 mg BID. LY3295668 had a manageable toxicity profile and demonstrated activity in some patients with locally advanced or metastatic solid tumors. Trial registration ClinicalTrials.gov, NCT03092934. Registered March 22, 2017. https://clinicaltrials.gov/ct2/show/NCT03092934 .

Published

2021

49. A phase I dose-escalation study of Selumetinib in combination with Erlotinib or Temsirolimus in patients with advanced solid tumors.

Author

Infante, Jeffrey, Cohen, Roger, Kim, Kevin, Burris, Howard, Curt, Gregory, Emeribe, Ugochi, Clemett, Delyth, Tomkinson, Helen, and LoRusso, Patricia

Subjects

ANTINEOPLASTIC agents, ERLOTINIB, COMBINATION drug therapy, CLINICAL trials, DIARRHEA, DOSE-effect relationship in pharmacology, ENZYME inhibitors, EXANTHEMA, FATIGUE (Physiology), NAUSEA, NEUTROPENIA, TUMORS, TREATMENT effectiveness, MUCOSITIS, THERAPEUTICS

Abstract

Background Combinations of molecularly targeted agents may provide optimal anti-tumor activity and improve clinical outcomes for patients with advanced cancers. Selumetinib (AZD6244, ARRY-142886) is an oral, potent and highly selective, allosteric inhibitor of MEK1/2, a component of the RAS/RAF/MEK/ERK pathway which is constitutively activated in many cancers. We investigated the safety, tolerability, and pharmacokinetics (PK) of selumetinib in combination with molecularly targeted drugs erlotinib or temsirolimus in patients with advanced solid tumors. Methods Two-part study: dose escalation, to determine the maximum tolerated dose (MTD) of selumetinib in combination with erlotinib 100 mg once daily (QD) or temsirolimus 25 mg once weekly, followed by dose expansion at the respective combination MTDs to further investigate safety and anti-tumor effects. Results 48 patients received selumetinib plus erlotinib and 32 patients received selumetinib plus temsirolimus. The MTD with erlotinib 100 mg QD was selumetinib 100 mg QD, with diarrhea being dose limiting. The most common all grade adverse events (AEs): diarrhea, rash, nausea, and fatigue. Four (8.3%) patients had ≥12 weeks stable disease. The MTD with temsirolimus 25 mg once weekly was selumetinib 50 mg twice daily (BID), with mucositis and neutropenia being dose limiting. The most commonly reported AEs: nausea, fatigue, diarrhea, and mucositis. Ten (31.3%) patients had ≥12 weeks stable disease. The combination PK profiles were comparable to previously observed monotherapy profiles. Conclusions MTDs were established for selumetinib in combination with erlotinib or temsirolimus. Overlapping toxicities prevented the escalation of selumetinib to its recommended phase II monotherapy dose of 75 mg BID. Trial registration: NCT00600496; registered 8 July 2009. [ABSTRACT FROM AUTHOR]

Published

2017

50. A first-in-human, phase 1, dose-escalation study of ABBV-176, an antibody-drug conjugate targeting the prolactin receptor, in patients with advanced solid tumors

Author

Peter Ansell, Nancy Chan, Bo Tong, Louie Naumovski, Jasgit C. Sachdev, Charlotte Lemech, Christine K. Ratajczak, Joanne E. Mortimer, Silpa Nuthalapati, Fang Jiang, and Natasha Woodward

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Immunoconjugates, Receptors, Prolactin, Colorectal cancer, Nausea, Antineoplastic Agents, Neutropenia, Gastroenterology, 03 medical and health sciences, 0302 clinical medicine, Breast cancer, Pharmacokinetics, Neoplasms, Internal medicine, Humans, Medicine, Pharmacology (medical), Adverse effect, Aged, Pharmacology, business.industry, Prolactin receptor, Middle Aged, medicine.disease, Treatment Outcome, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Toxicity, Female, medicine.symptom, business

Abstract

ABBV-176 is an antibody-drug conjugate composed of the humanized antibody h16f (PR-1594804) conjugated to a highly potent, cytotoxic cross-linking pyrrolobenzodiazepine dimer (PBD; SGD-1882) targeting the prolactin receptor (PRLR), which is overexpressed in several solid tumor types. This phase 1, dose-escalation study (NCT03145909) evaluated the safety, pharmacokinetics, and preliminary activity of ABBV-176 in patients with advanced solid tumors likely to exhibit elevated levels of PRLR. Patients received ABBV-176 once every 3 weeks. Dose escalation was by an exposure-adjusted, continual reassessment method. Dose-limiting toxicities (DLTs) were assessed from the first day of dosing until the next dose of ABBV-176 to determine the maximum tolerated dose (MTD) and recommended phase 2 dose (RP2D). Nineteen patients received ABBV-176 at doses from 2.7-109.35 μg/kg. Patients enrolled had colorectal cancer (n = 11), breast cancer (n = 6), or adrenocortical carcinoma (n = 2). DLTs occurred in 4 patients and included thrombocytopenia (n = 2; both at 99.9-μg/kg dose level), neutropenia (n = 2; 78.3-μg/kg and 99.9-μg/kg dose levels), and pancytopenia (n = 1; 109.35-μg/kg dose level). The most common treatment-emergent adverse events related to ABBV-176 were thrombocytopenia, neutropenia, increased aspartate aminotransferase, nausea, fatigue, and pleural effusions. Effusions and edema were common, and timing of onset suggested possible cumulative ABBV-176 toxicity. Tumor expression of PRLR varied among patients enrolled and analyzed. No patient had an objective response. MTD was not formally determined, as identification of a tolerable dose was confounded by late-onset toxicities. ABBV-176 was associated with significant toxicity in this phase 1, dose-escalation study. Although cytopenias were often dose limiting, effusions and edema were also common and had late onset that suggested cumulative toxicity. No responses were observed, although data were available from a small number of patients with variable tumor PRLR expression. This study was terminated after the dosing of 19 patients.

Published

2020