Your search keyword '"Peixoto, Fábio"' showing total 3 results

1. Use of topical rSm29 in combination with intravenous meglumine antimoniate in the treatment of cutaneous leishmaniasis: A randomized controlled trial.

Author

Lago, Tainã, Peixoto, Fábio, Mambelli, Fábio, Carvalho, Lucas P., Guimarães, Luiz Henrique, Carvalho, Augusto M., Cardoso, Luciana, Machado, Paulo R.L., Scott, Phillip, Lago, Jamile, Andrade, Juvana M., Fahel, Júlia S., Oliveira, Sérgio C., and Carvalho, Edgar M.

Subjects

*CUTANEOUS leishmaniasis, *SCHISTOSOMA mansoni, *CLINICAL trials, *RANDOMIZED controlled trials, *GRANZYMES

Abstract

• Cutaneous leishmaniasis due to L. braziliensis has a high rate of failure to therapy. Severity of the disease and failure to therapy is associated with Granzyme B level. • Recombinant Sm29 (rSm29) down-modulate Granzyme B production. • Antimony in combination with rSm29 increases the cure rate of cutaneous leishmaniasis. Cutaneous leishmaniasis (CL) caused by Leishmania (Viannia) braziliensis is associated with an inflammatory response. Granzyme (GzmB) and IL-1β play a key role in the pathology. Meglumine antimoniate (MA) is the first-choice drug for the treatment of CL, but therapy failure is observed in up to 50% of the cases. The protein, rSm29 of Schistosoma mansoni , down-modulates pro-inflammatory cytokine production. We evaluate if the combination of topical rSm29 plus MA increases the cure rate of CL. In this randomized clinical trial, 91 CL patients were allocated in 3 groups. All cases received MA (20 mg/kg/weight) for 20 days. Group 1 used topical rSm29 (10 µg), group 2 a placebo topically applied, and group 3 received only MA. The cure rate on day 90 was 71% in subjects treated with rSm29 plus MA, and 43% in patients who received MA plus placebo or MA alone (P < 0.05). There was a decrease in GzmB and an increase in IFN-γ (P < 0.05) in supernatants of skin biopsies of the lesions obtained on D7 of therapy (P < 0.05) in patients who received rSm29. rSm29 associated with MA reduces GzmB levels, is more effective than MA alone, and decreases CL healing time. ClinicalTrial.gov under NCT06000514. [ABSTRACT FROM AUTHOR]

Published

2024

2. A phase 2 randomized clinical trial of abiraterone plus ADT, apalutamide, or abiraterone and apalutamide in patients with advanced prostate cancer with non-castrate testosterone levels (LACOG 0415).

Author

Maluf, Fernando C., Schutz, Fabio A., Cronemberger, Eduardo H., Luz, Murilo de A., Martins, Suelen P.S., Muniz, David Q.B., Bastos, Diogo A., Cárcano, Flavio M., Smaletz, Oren, Soares, Andrey, Peixoto, Fábio A., Gomes, Andrea J., Cruz, Felipe M., Franke, Fabio A., Herchenhorn, Daniel, dos Santos, Telma M., Fabricio, Vanessa de C., Gidekel, Rosemarie, Werutsky, Gustavo, and de Jesus, Rafaela G.

Subjects

*THERAPEUTIC use of antineoplastic agents, *ANTIANDROGENS, *CONFIDENCE intervals, *GOSERELIN, *TESTOSTERONE, *ABIRATERONE acetate, *CANCER relapse, *METASTASIS, *HEALTH status indicators, *TREATMENT effectiveness, *RANDOMIZED controlled trials, *DESCRIPTIVE statistics, *QUALITY of life, *STATISTICAL sampling, *PROSTATE-specific antigen, *DRUG side effects, *PREDNISONE, *PROSTATE tumors

Abstract

Androgen deprivation therapy (ADT) combined with apalutamide, abiraterone acetate plus prednisone, enzalutamide, or docetaxel are the standard treatments for advanced castration-sensitive prostate cancer (CSPC). We investigated ADT-free alternatives for advanced CSPC. LACOG 0415 is a phase 2, open-label, non-comparative, randomized trial. Patients with advanced CSPC were randomized (1:1:1) to receive goserelin plus abiraterone acetate and prednisone (ADT plus AAP arm), apalutamide (APA arm), or apalutamide plus abiraterone acetate and prednisone (APA plus AAP arm). The primary endpoint was the proportion of patients with PSA of ≤0.2 ng/mL at week 25 in the modified intention-to-treat population. Safety analyses were performed in all patients with at least one dose of the study drug. Of 128 randomized patients, 120 patients were evaluable for PSA response at week 25; 17.2% had a high-risk biochemical recurrence, 8.6% had locally advanced disease, and 74.2% had distant metastases. At week 25, PSA of ≤0.2 ng/mL was observed in 75.6% (95%CI 59.7%–87.6%), 60.0% (95%CI 43.3%–75.1%), and 79.5% (95%CI 63.5%–90.7%) of patients in ADT plus AAP, APA, and APA plus AAP arms, respectively. PSA decline of ≥80% was observed in 100%, 90.0%, and 97.4%, respectively. Grade 3–4 AEs were observed in 31.0%, 21.4% and 36.4%, respectively. Testosterone levels increased significantly in the APA arm and decreased significantly in ADT plus AAP and APA plus AAP arms. ADT-free alternatives provide a high PSA response in advanced CSPC, although the APA arm did not reach the expected rate of PSA of ≤0.2 ng/mL at week 25. These results warrant further investigation of ADT-free treatments as alternatives in advanced CSPC. ClinicalTrials.gov NCT02867020. • ADT-free alternatives provide high PSA response in advanced CSPC. • Although the APA arm did not reach the expected rate of PSA of ≤0.2 ng/mL at week 25. • The three arms had a distinct toxicity profile and similar HRQoL. [ABSTRACT FROM AUTHOR]

Published

2021

3. XAF1 mRNA expression improves progression-free and overall survival for patients with advanced bladder cancer treated with neoadjuvant chemotherapy

Author

Pinho, Marcos B., Costas, Fernanda, Sellos, João, Dienstmann, Rodrigo, Andrade, Patricia B., Herchenhorn, Daniel, Peixoto, Fábio Afonso, Santos, Valdelice O., Small, Isabele A., Guimarães, Denise P., and Ferreira, Carlos G.

Subjects

*APOPTOSIS, *CHEMICAL inhibitors, *MESSENGER RNA, *GENE expression, *SURVIVAL analysis (Biometry), *BLADDER cancer, *CANCER chemotherapy, *CANCER patients, *TUMOR suppressor genes, *PROGNOSIS

Abstract

Abstract: Purpose: The aim of this study was to investigate whether mRNA expression of the apoptosis-associated genes, XAF1 and XIAP, in bladder cancer patients correlates with response to neoadjuvant treatment. Methods: Gene expression was analyzed by a real-time quantitative PCR method in paired samples from 14 bladder cancer patients treated with a combination of neoadjuvant gemcitabine and cisplatin. The prognostic significance of XAF1 and XIAP mRNA expression as well as the correlation with several clinical and pathological findings were evaluated. Results: The clinical response in the XAF1-high subset (n = 5) was remarkably higher compared with the XAF1-low subset (n = 9) (100% vs. 44.4%; P = 0.038). These results translated into a notably improvement of progression-free survival (PFS) in the XAF1-high subset (log-rank P = 0.012). In addition, patients in the XAF1-high subset had a 3.9-fold decreased chance of dying from the disease (hazard ratio for death (HR), 0.257; (CI 95%), 0.043–1.536, P = 0.036). When we evaluated the expression of XIAP, although an inverse correlation was found between expression and pathological response, there were no statistically significant associations with the clinical response, the length of PFS, and OS. Conclusions: This is one of the few studies to address the role of XAF1 in a clinical setting. The data presented here identify XAF1 as a novel predictive and prognostic factor in bladder cancer patients. Furthermore, our observations are in line with previous studies, which point towards XAF1 as a tumor-suppressor gene. Nonetheless, additional studies, both mechanistic and translational, are warranted and may help not only in corroborating the role of XAF1 as a prognostic marker, but also as a potential target for anticancer therapy. [Copyright &y& Elsevier]

Published

2009