Background: Phase 3 studies have shown long-acting (LA) cabotegravir/rilpivirine to be effective and tolerable as maintenance therapy in people with HIV (PWH). However, real-life data on their effectiveness are limited. Methods: All PWH enrolled in the Icona Cohort who started LA cabotegravir/rilpivirine with HIV-RNA < 50 copies/mL were included. Times to treatment discontinuation (TD) and to virological failure (VF50, two consecutive HIV-RNA >50 copies/mL or one >1000 copies/mL followed by ART switch) were estimated by the Kaplan–Meier method. Cox regression models, adjusted for age, sex and mode of HIV transmission and stratified by the centre, were employed. Results: Overall, 583 PWH started LA cabotegravir/rilpivirine. Six VF50 were observed, with a 1 year estimated cumulative probability of virological failure of 1.2% (95% CI, 0.5%–3.0%). Resistance-associated mutations for rilpivirine and cabotegravir were detected in 3/4 and 4/4 participants with VF50, respectively, for which the genotypic resistance test was performed. The 1 year cumulative probability of TD was 11.4% (95% CI, 8.6%–14.9%), mainly caused by toxicity/adverse events (73.2%). Multivariable analysis identified heterosexual intercourse and IV drug use as significant risk factors for TD compared with MSM. Conclusions: This analysis demonstrated the short-term effectiveness of cabotegravir/rilpivirine in a real-life setting showing minimal incidence of virological failure but a notable probability of discontinuation due to toxicity or adverse events.
Effectiveness and predictors of treatment discontinuation of long-acting cabotegravir/rilpivirine in virologically suppressed people with HIV: real-life data from the Icona Cohort / R. Gagliardini, S. De Benedittis, A. Tavelli, G. Lapadula, V. Mazzotta, E. Bruzzesi, A. Cervo, G. Carrozzo, A. Saracino, S. Rusconi, G. Marchetti, F. Ceccherini-Silberstein, A. Antinori, A. D'Arminio Monforte, C. Muccini, S. Antinori, A. Castagna, R. Cauda, G. Di Perri, E. Girardi, R. Iardino, A. Lazzarin, G. C Marchetti, C. Mussini, E. Quiros-Roldan, L. Sarmati, B. Suligoi, F. Von Schloesser, P. Viale, A. Cingolani, A. Cozzi-Lepri, A. Di Biagio, A. Gori, S. Lo Caputo, G. Marchetti, F. Maggiolo, M. Puoti, C. F Perno, C. Torti, A. Bandera, S. Bonora, A. Calcagno, D. Canetti, P. Cinque, A. Cozzi-Lepri, A. Di Biagio, A. Giacomelli, E. Girardi, N. Gianotti, G. Guaraldi, S. Lanini, M. Lichtner, A. Lai, S. Lo Caputo, G. Madeddu, V. Malagnino, A. Mondi, S. Nozza, S. Piconi, C. Pinnetti, M. Puoti, R. Rossotti, M. M Santoro, L. Sarmati, V. Spagnuolo, N. Squillace, V. Svicher, L. Taramasso, A. Vergori, A. Cozzi-Lepri, I. Fanti, M. Giotta, C. Marelli, A. Rodano, M. Cernuschi, L. Cosmaro, A. Perziano, V. Calvino, D. Russo, M. Farinella, N. Policek, V. L Del Negro, M. Augello, S. Carrara, S. Graziano, G. Prota, S. Truffa, D. Vincenti, R. Rovito, H. Sadeghi, A. Giacometti, A. Costantini, V. Barocci, C. Santoro, E. Milano, L. Comi, C. Suardi, P. Viale, L. Badia, S. Cretella, E. M Erne, A. Pieri, E. Focà, B. Menzaghi, C. Abeli, L. Chessa, F. Pes, P. Maggi, L. Alessio, G. Nunnari, B. M Celesia, J. Vecchiet, K. Falasca, A. Pan, S. Dal Zoppo, D. Segala, F. Bartalesi, C. Costa, S. Lo Caputo, S. Ferrara, M. Bassetti, E. Pontali, S. Blanchi, N. Bobbio, C. Del Borgo, R. Marocco, G. Mancarella, C. Molteni, G. Canavesi, G. Pellicanò, G. Rizzardini, M. Puoti, V. Bono, M. V Cossu, R. Lolatto, M. C Moioli, L. Pezzati, S. Diotallevi, C. Tincati, M. Menozzi, P. Bonfanti, V. Sangiovanni, I. Gentile, V. Esposito, N. Coppola, F. M Fusco, G. Di Filippo, V. Rizzo, N. Sangiovanni, S. Martini, A. M Cattelan, D. Leoni, A. Cascio, M. Trizzino, D. Francisci, E. Schiaroli, G. Parruti, F. Sozio, D. Messeri, S. I Bonelli, C. Lazzaretti, R. Corsini, R. Cauda, C. Mastroianni, L. Sarmati, A. Latini, I. Mastrorosa, S. Lamonica, M. Capozzi, M. Camici, I. Mezzaroma, M. Rivano Capparuccia, G. Iaiani, C. Stingone, L. Gianserra, J. Paulicelli, M. M Plazzi, G. D'Ettore, M. Fusto, I. Coledan, G. Madeddu, A. De Vito, M. Fabbiani, F. Montagnani, A. Franco, R. Fontana Del Vecchio, D. Francisci, C. Di Giuli, G. C Orofino, G. Calleri, G. Di Perri, G. Accardo, C. Tascini, A. Londero, G. Battagin, S. Nicolè, G. Starnini, S. Dell'Isola. - In: JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY. - ISSN 0305-7453. - 80:8(2025 Aug 01), pp. 2169-2178. [10.1093/jac/dkaf184]
Effectiveness and predictors of treatment discontinuation of long-acting cabotegravir/rilpivirine in virologically suppressed people with HIV: real-life data from the Icona Cohort
S. Rusconi;G. Marchetti;A. D'Arminio Monforte;S. Antinori;A. Bandera;A. Giacomelli;M. Augello;A. Pan;C. Tincati;
2025
Abstract
Background: Phase 3 studies have shown long-acting (LA) cabotegravir/rilpivirine to be effective and tolerable as maintenance therapy in people with HIV (PWH). However, real-life data on their effectiveness are limited. Methods: All PWH enrolled in the Icona Cohort who started LA cabotegravir/rilpivirine with HIV-RNA < 50 copies/mL were included. Times to treatment discontinuation (TD) and to virological failure (VF50, two consecutive HIV-RNA >50 copies/mL or one >1000 copies/mL followed by ART switch) were estimated by the Kaplan–Meier method. Cox regression models, adjusted for age, sex and mode of HIV transmission and stratified by the centre, were employed. Results: Overall, 583 PWH started LA cabotegravir/rilpivirine. Six VF50 were observed, with a 1 year estimated cumulative probability of virological failure of 1.2% (95% CI, 0.5%–3.0%). Resistance-associated mutations for rilpivirine and cabotegravir were detected in 3/4 and 4/4 participants with VF50, respectively, for which the genotypic resistance test was performed. The 1 year cumulative probability of TD was 11.4% (95% CI, 8.6%–14.9%), mainly caused by toxicity/adverse events (73.2%). Multivariable analysis identified heterosexual intercourse and IV drug use as significant risk factors for TD compared with MSM. Conclusions: This analysis demonstrated the short-term effectiveness of cabotegravir/rilpivirine in a real-life setting showing minimal incidence of virological failure but a notable probability of discontinuation due to toxicity or adverse events.
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