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Your search keyword '"Prasant, Mohanty"' showing total 6 results
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6 results on '"Prasant, Mohanty"'

2. Best ablation strategy in patients with premature ventricular contractions with multiple morphology: a single-centre experience

Author

Sanghamitra Mohanty, John D Burkhardt, Luigi Di Biase, Prasant Mohanty, Sai Shishir Shetty, Carola Gianni, Domenico G Della Rocca, Karim K Baho, Trevor Morris, Angel Mayedo, Bryan MacDonald, Amin Al-Ahmad, Mohamed Bassiouny, Gerald Joseph Gallinghouse, Rodney Horton, and Andrea Natale

Subjects
Physiology (medical), Cardiology and Cardiovascular Medicine
Abstract

AimsThis study aimed to examine the clinical benefits of targeted ablation of all Premature ventricular complex (PVC) morphologies vs. predominant PVC only.Methods and resultsA total of 171 consecutive patients with reduced left ventricular ejection fraction (LVEF) and ≥2 PVC morphology with high burden (>10%/day) undergoing their first ablation procedure were included in the analysis. At the initial procedure, prevalent PVC alone was ablated in the majority. However, at the redo, all PVC morphologies were targeted for ablation. : At the first procedure, 152 (89%) patients received ablation of the dominant PVC only. In the remaining 19 (11%) patients, all PVC morphologies were ablated. At two years, high PVC burden was detected in 89 (52%) patients. Repeat procedure was performed in 78 of 89, where all PVC morphologies were ablated. At 5 years after the repeat procedure, 71 (91%) had PVC burden of ConclusionIn this observational series, ablation of all PVC morphologies was associated with significantly lower PVC burden and improvement of LVEF at long-term follow-up, compared with ablation of the dominant morphology only.

Published
2023
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5. OUTCOME OF DIFFERENT ABLATION STRATEGIES IN PERSISTENT AND LONG-STANDING PERSISTENT ATRIAL FIBRILLATION: RESULTS FROM A MULTICENTER RANDOMIZED TRIAL (TANTRA)

Author

Sanghamitra Mohanty, Prasant Mohanty, Chintan Trivedi, Michela Casella, Antonio Dello Russo, Paolo Compagnucci, Domenico Giovanni Della Rocca, Carola Gianni, Paolo China, Sakis Themistoclakis, Bryan MacDonald, Angel Mayedo, Amin Al-Ahmad, Rodney P. Horton, Mohamed Bassiouny, Gerald Gallinghouse, John Burkhardt, Luigi Di Biase, Claudio Tondo, and Andrea Natale

Subjects
Cardiology and Cardiovascular Medicine
Published
2022
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6. Ezabenlimab (BI 754091), an anti-PD-1 antibody, in combination with BI 836880, a VEGF/Ang2-blocking nanobody, in patients (pts) with advanced colorectal cancer (CRC)

Author

Susanna Varkey Ulahannan, Ivor John Percent, Edward Arrowsmith, Maen A. Hussein, Viralkumar K. Bhanderi, John Hamm, Greg Andrew Durm, Damijan Erzen, Prasant Mohanty, and David R. Spigel

Subjects
Cancer Research, Oncology
Abstract

98 Background: Anti-PD-1 antibodies may have synergistic effects with other immunomodulatory or targeted agents. This open-label, Phase II platform trial is investigating ezabenlimab, an anti-PD-1 antibody, combined with other agents. Module C of the platform is assessing ezabenlimab plus BI 836880, a humanized bispecific nanobody targeting VEGF/Ang2. Pts are being enrolled into 5 advanced solid tumor cohorts: gastric/gastroesophageal adenocarcinoma; solid tumors (except non-squamous NSCLC or melanoma) with secondary resistance to anti-PD-(L)1 treatment (progression after at least SD for ≥4 months); solid tumors with primary resistance to anti-PD-(L)1 treatment; microsatellite stable (MSS) CRC; mismatch repair-proficient/MSS endometrial carcinoma. Here, we report data from the CRC cohort which has completed recruitment. Methods: Pts with locally advanced, unresectable or metastatic, MSS CRC were enrolled. Patients had received ≥1 line of prior systemic therapy for metastatic disease but were anti-PD-(L)-1 therapy-naïve. Prior anti-angiogenic therapy was permitted. Pts received BI 836880 720 mg plus ezabenlimab 240 mg iv q3w for 1 year or until disease progression, consent withdrawal or undue toxicity. Primary endpoint: investigator-assessed OR (CR or PR per RECIST v1.1). Secondary endpoints: duration of response, disease control, and PFS; safety is also being assessed. Results: 30 pts have been treated: 57% male; median age 61.5 years. All pts had received prior chemotherapy; most pts (23 [77%]) had received prior bevacizumab. At data cut-off (Sep 2021), median duration (range) of treatment was 115.5 (28–295) days; 6 pts remain on treatment. 1 (3%) pt (who had not received prior bevacizumab) achieved a confirmed PR; 16 (53%) pts had SD. Median duration (range) of SD was 128.5 (42–242) days. 29/17/2 (97/57/7%) pts had an AE (any/G3/G4). The most frequent AEs (any/G3) were nausea (40/10%), fatigue (30/3%), peripheral edema (30/0%), vomiting (27/7%), and hypertension (27/17%). There were two G4 AEs (hypertension; platelet count decreased) and no G5 AEs. 24/10/2 (80/33/7%) pts had a drug-related AE (any/G3/G4); most commonly (any/G3) nausea (33/7%), fatigue (27/3%) and hypertension (27/17%). 3 (10%) pts had an infusion-related reaction (G1, n = 1; G2, n = 2). 2 (7%) pts had an AE leading to discontinuation (G3 bile duct stone and G2 peripheral edema). Immune-related AEs were reported in 6 (20%) pts and serious AEs occurred in 13 (43%) pts. Conclusions: BI 836880 plus ezabenlimab had a manageable safety profile in pts with advanced MSS CRC; however, anti-tumor activity was limited in these pts, the majority of whom had received prior bevacizumab. Clinical trial information: NCT03697304.

Published
2022
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