BackgroundAutophagy is the primary catabolic process responsible for degrading intracellular components and potentially harmful cytosolic entities by delivering them to lysosomes. Notably, this mechanism is crucial for controlling intracellular pathogens, with significant implications for both innate and adaptive immunity. In the context of HIV-1 infection, emerging evidence suggests that autophagy contributes to immune responses against the virus. Various compounds can modulate autophagy, among which vitamin D-3 is particularly effective due to its ability to prevent inflammation and slow HIV-1 disease progression. Indeed, vitamin D-3 contributes to regulating both innate and adaptive immunity, thereby modulating antiviral and antibacterial inflammatory responses. Importantly, vitamin D-3 deficiency is highly prevalent among people with HIV (PWH) and has been associated with an increased risk of severe disease progression.ResultsIn this study, we investigated the relationship between serum vitamin D-3 levels and the expression of autophagy markers in peripheral blood mononuclear cells from different categories of PWH: PWH under antiretroviral therapy (ART) with either normal vitamin D-3 levels or hypovitaminosis, and treatment-na & iuml;ve PWH with either normal vitamin D-3 levels or hypovitaminosis. Our results show that low vitamin D-3 blood levels is associated with lower expression of the main factors involved in the autophagy mechanism, particularly in treatment-na & iuml;ve PWH.ConclusionsOur findings suggest that normal blood level of vitamin D-3 may play a crucial role in promoting autophagy in PWH. The observed differences in autophagy-related protein expression between ART-treated and untreated individuals underscore the intricate relationship between vitamin D-3 levels, ART exposure, and autophagic regulation. This is a preliminary exploration of the effects of vitamin D-3 on autophagy in PWH. Further studies are needed to deepen and explore the interplay between vitamin D-3 and autophagy in greater depth. A better understanding of these mechanisms could help to develop novel therapeutic strategies aimed at mitigating immune depletion and chronic inflammation, ultimately improving clinical outcomes for individuals living with HIV.
Casetti, R., Ciccosanti, F., Lamsira, H.K., Pinnetti, C., Mazzotta, V., Ciolfi, S., et al. (2025). Autophagy is influenced by vitamin D3 level in people with HIV-1. BIOLOGY DIRECT, 20(1) [10.1186/s13062-025-00660-9].
Autophagy is influenced by vitamin D3 level in people with HIV-1
Ciolfi S.;Piacentini M.;Nardacci R.
2025-01-01
Abstract
BackgroundAutophagy is the primary catabolic process responsible for degrading intracellular components and potentially harmful cytosolic entities by delivering them to lysosomes. Notably, this mechanism is crucial for controlling intracellular pathogens, with significant implications for both innate and adaptive immunity. In the context of HIV-1 infection, emerging evidence suggests that autophagy contributes to immune responses against the virus. Various compounds can modulate autophagy, among which vitamin D-3 is particularly effective due to its ability to prevent inflammation and slow HIV-1 disease progression. Indeed, vitamin D-3 contributes to regulating both innate and adaptive immunity, thereby modulating antiviral and antibacterial inflammatory responses. Importantly, vitamin D-3 deficiency is highly prevalent among people with HIV (PWH) and has been associated with an increased risk of severe disease progression.ResultsIn this study, we investigated the relationship between serum vitamin D-3 levels and the expression of autophagy markers in peripheral blood mononuclear cells from different categories of PWH: PWH under antiretroviral therapy (ART) with either normal vitamin D-3 levels or hypovitaminosis, and treatment-na & iuml;ve PWH with either normal vitamin D-3 levels or hypovitaminosis. Our results show that low vitamin D-3 blood levels is associated with lower expression of the main factors involved in the autophagy mechanism, particularly in treatment-na & iuml;ve PWH.ConclusionsOur findings suggest that normal blood level of vitamin D-3 may play a crucial role in promoting autophagy in PWH. The observed differences in autophagy-related protein expression between ART-treated and untreated individuals underscore the intricate relationship between vitamin D-3 levels, ART exposure, and autophagic regulation. This is a preliminary exploration of the effects of vitamin D-3 on autophagy in PWH. Further studies are needed to deepen and explore the interplay between vitamin D-3 and autophagy in greater depth. A better understanding of these mechanisms could help to develop novel therapeutic strategies aimed at mitigating immune depletion and chronic inflammation, ultimately improving clinical outcomes for individuals living with HIV.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
