Your search keyword '"Silvana Mouron"' showing total 2 results

1. A randomized phase 0 trial of the mitochondrial inhibitor ME344 or placebo added to the antiangiogenic (Aa) bevacizumab in early HER2-negative breast cancer (E-HERNEBC)

Author

Javier Cortes, Luis Manso, Serafin Morales, Juan V. Apala, Alfonso Cortés Salgado, Francisca Mulero, Eduardo Caleiras, Silvana Mouron, Miguel Quintela-Fandino, and Juan Antonio Guerra

Subjects

Cancer Research, Bevacizumab, business.industry, HER2 negative, Metabolism, Pharmacology, Vascular normalization, Placebo, medicine.disease, Breast cancer, Oncology, medicine, business, medicine.drug

Abstract

3100 Background: We have shown that when Aas induce vascular normalization (VN), tumors escape upregulating mitochondrial metabolism. Mitochondrial inhibition with ME344 induced synergy with various Aas. We also found that VN could be traced by showing a 10% decrease in tumor FDG-PET SUV from day (d) 0 to d8 of Aa. We studied the activity of adding ME344 or placebo to Bev (Ki67 decrease) in E-HERNEBC in a phase 0 randomized trial. As a secondary objective we measured the activity of the combination in patients (Pts) showing VN according to FDG-PET. Methods: Untreated E-HERNEBC Pts with T > 1cm, any N, M0 underwent a baseline FDG-PET (d1) and received a single dose of Bev (15mg/kg) prior to randomization (1:1) to arm A (FDG-PET on d8 followed by ME344 10 mg/kg IV on d8, d15 and d21) or Arm B (FDG-PET on d8 followed by placebo on d8, d15 and d21). Tumors were biopsied on d0 and 28. A 40 Pts sample size was powered to detect a 30% relative difference between arms in digitally acquired Ki67 decrease from d0 to d28 (alpha 0.05, beta 0.2). Results: Arm A: 20 Pts; Arm B: 21 Pts. Baseline characteristics were in arm A vs B: age 58.4(41.5-75.3) vs 53.6(39-82.8); T1(30%)/T2(60%)/T3(10%) vs T1(52%)/T2(48%)/T3(0%); N0(80%)/N1(20%) vs N0(81%)/N1(19%); ER+(75%)/TNBC(25%) vs ER+(71.4%)/TNBC(28.6%); Ki67 31.6% (3.6%-70%) vs 25.2% (1.2% - 81.5%). PET-SUV decreased > 10% from d0 to d8 in 6/20 (arm A) and 6/21 (arm B) Pts. Two G3 adverse events (blood pressure) were reported (1/arm) and deemed related to Bev. Results of the primary endpoint: table. Conclusions: ME344 showed significant biologic activity, enhancing the effect in Ki67 decrease vs placebo when added to Bev in E-HERNEBC. The activity was greater in TNBC. A trend for greater activity in patients experiencing VN according to FDG-PET was observed. Clinical trial information: NCT02806817. [Table: see text]

Published

2019

2. Abrogation of resistance against bevacizumab (Bev) by mitochondrial inhibition: A phase 0 randomized trial of Bev plus ME344 or placebo in early HER2-negative breast cancer (HERNEBC)

Author

Juan V. Apala, Alfonso Cortés Salgado, Silvana Mouron, Mana Gion Cortes, Juan Antonio Guerra, Miguel Quintela-Fandino, M.M. Morente, and Luis Manso

Subjects

0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Bevacizumab, Placebo, law.invention, 03 medical and health sciences, 0302 clinical medicine, Acquired resistance, Breast cancer, Randomized controlled trial, law, Internal medicine, medicine, business.industry, HER2 negative, Hypoxia (medical), medicine.disease, Preclinical data, 030104 developmental biology, 030220 oncology & carcinogenesis, medicine.symptom, business, medicine.drug

Abstract

2552Background: Our preclinical data show that one mechanism of acquired resistance to anti-angiogenic therapy involves hypoxia correction, measured by decreased SUV ( ↓ SUV) on FDG-PET followed by...

Published

2018