Background: Dyslipidemia represents a significant non-infectious comorbidity among people living with HIV. The aim of this study is to evaluate the impact on lipid profile of switches from an efavirenz (EFV) or protease inhibitor/ritonavir (PI/r)-based regimen to a rilpivirine (RPV) or a once-daily integrase inhibitor-based regimen. Methods: We analyzed data from SCOLTA prospective database. All patients with HIV-RNA < 50 copies/ml in therapy with two NRTI + EFV or PI/r were included if they switched from EFV to dolutegravir (group EFV-DTG), elvitegravir (EFV-EVG), or RPV (EFV-RPV) and from PI/r to DTG (PI/r-DTG), PI/r to EVG (PI/r-EVG), or PI/r to RPV (PI/r-RPV). Total cholesterol (TC), TC/HDL ratio, LDL-cholesterol (LDL) and triglycerides (TG) were compared at baseline, six months and one year. Comparisons among groups were performed by a general linear model. Results: Four hundred and ninety patients were enrolled, 24.9% female, mean age 47.3 years (±10.1). According to ART switch, 11.4% were classified in group EFV-DTG, 3.9% in EFV-EVG, 23.9% in EFV-RPV, 17.6% in PI/r-DTG, 17.8% in PI/r-EVG, and 25.5% in PI/r-RPV. After adjusted analysis, TC significantly decreased in all groups but EFV-EVG, TC/HDL in all but EFV-DTG and EFV-EVG, while the reduction of TG was significant only in switches to RPV (EFV-RPV and PI/r-RPV). The one year decrease of TC, TC/HDL, LDL and TG was higher in patients with higher baseline levels of the same variable (p < .0001 for all). Conclusions: In SCOLTA, all switches from PI/r regimens gave advantages on lipid profile, while stopping EFV had consistently favorable lipid effects only if replaced by RPV.

Improvement of lipid profile after switching from efavirenz or ritonavir-boosted protease inhibitors to rilpivirine or once-daily integrase inhibitors: Results from a large observational cohort study (SCOLTA) / Taramasso, L.; Tatarelli, P.; Ricci, E.; Madeddu, G.; Menzaghi, B.; Squillace, N.; De Socio, G. V.; Martinelli, C.; Gulminetti, R.; Maggi, P.; Orofino, G.; Vichi, F.; Di Biagio, A.; Bonfanti, P.; Bellacosa, C.; Calza, L.; Abeli, C.; Celesia, B. M.; Grosso, C.; Stagno, A.; Mazzotta, F.; Penco, G.; Cassola, G.; Nicolini, L. A.; Dentone, C.; Molteni, C.; Palvarini, L.; Scalzini, A.; Carenzi, L.; Rizzardini, G.; Valsecchi, L.; Cordier, L.; Rusconi, S.; Colombo, V.; Galli, M.; Franzetti, M.; Sgrelli, A.; Mazzotta, E.; Parruti, G.; Bagella, P.; Mura, M. S.; Libertone, R.; Antinori, A.; Di Giambenedetto, S.; Guastavigna, M.; Caramello, P.. - In: BMC INFECTIOUS DISEASES. - ISSN 1471-2334. - 18:1(2018), p. 357. [10.1186/s12879-018-3268-5]

Improvement of lipid profile after switching from efavirenz or ritonavir-boosted protease inhibitors to rilpivirine or once-daily integrase inhibitors: Results from a large observational cohort study (SCOLTA)

Madeddu G.;
2018-01-01

Abstract

Background: Dyslipidemia represents a significant non-infectious comorbidity among people living with HIV. The aim of this study is to evaluate the impact on lipid profile of switches from an efavirenz (EFV) or protease inhibitor/ritonavir (PI/r)-based regimen to a rilpivirine (RPV) or a once-daily integrase inhibitor-based regimen. Methods: We analyzed data from SCOLTA prospective database. All patients with HIV-RNA < 50 copies/ml in therapy with two NRTI + EFV or PI/r were included if they switched from EFV to dolutegravir (group EFV-DTG), elvitegravir (EFV-EVG), or RPV (EFV-RPV) and from PI/r to DTG (PI/r-DTG), PI/r to EVG (PI/r-EVG), or PI/r to RPV (PI/r-RPV). Total cholesterol (TC), TC/HDL ratio, LDL-cholesterol (LDL) and triglycerides (TG) were compared at baseline, six months and one year. Comparisons among groups were performed by a general linear model. Results: Four hundred and ninety patients were enrolled, 24.9% female, mean age 47.3 years (±10.1). According to ART switch, 11.4% were classified in group EFV-DTG, 3.9% in EFV-EVG, 23.9% in EFV-RPV, 17.6% in PI/r-DTG, 17.8% in PI/r-EVG, and 25.5% in PI/r-RPV. After adjusted analysis, TC significantly decreased in all groups but EFV-EVG, TC/HDL in all but EFV-DTG and EFV-EVG, while the reduction of TG was significant only in switches to RPV (EFV-RPV and PI/r-RPV). The one year decrease of TC, TC/HDL, LDL and TG was higher in patients with higher baseline levels of the same variable (p < .0001 for all). Conclusions: In SCOLTA, all switches from PI/r regimens gave advantages on lipid profile, while stopping EFV had consistently favorable lipid effects only if replaced by RPV.
2018
Improvement of lipid profile after switching from efavirenz or ritonavir-boosted protease inhibitors to rilpivirine or once-daily integrase inhibitors: Results from a large observational cohort study (SCOLTA) / Taramasso, L.; Tatarelli, P.; Ricci, E.; Madeddu, G.; Menzaghi, B.; Squillace, N.; De Socio, G. V.; Martinelli, C.; Gulminetti, R.; Maggi, P.; Orofino, G.; Vichi, F.; Di Biagio, A.; Bonfanti, P.; Bellacosa, C.; Calza, L.; Abeli, C.; Celesia, B. M.; Grosso, C.; Stagno, A.; Mazzotta, F.; Penco, G.; Cassola, G.; Nicolini, L. A.; Dentone, C.; Molteni, C.; Palvarini, L.; Scalzini, A.; Carenzi, L.; Rizzardini, G.; Valsecchi, L.; Cordier, L.; Rusconi, S.; Colombo, V.; Galli, M.; Franzetti, M.; Sgrelli, A.; Mazzotta, E.; Parruti, G.; Bagella, P.; Mura, M. S.; Libertone, R.; Antinori, A.; Di Giambenedetto, S.; Guastavigna, M.; Caramello, P.. - In: BMC INFECTIOUS DISEASES. - ISSN 1471-2334. - 18:1(2018), p. 357. [10.1186/s12879-018-3268-5]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11388/218993
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