Reduction in the risk of progression of solid organ transplant recipients infected by SARS-CoV-2 treated with monoclonal antibodies / Reducción del riesgo de progresión en receptores de trasplantes infectados por SARS-CoV-2 tratados con anticuerpos monoclonales

Recipients of solid organ transplants (SOT) are at higher risk of infection by SARS-CoV-2 virus especially due to chronic immunosuppression therapy and frequent multiple comorbid conditions. COVID-19 is a potentially life-threatening disease in SOT recipients, with an increased likelihood of progressing to severe disease, with the need of hospitalization, admission to the intensive care unit (ICU) and mechanical ventilatory support. This article presents an updated review of different aspects related to the outcome of COVID-19 in SOT recipients. In nvaccinated SOT recipients, COVID-19 is associated with a high mortality rate, in-patient care and ICU admission, and impaired graft function or rejection in severe disease. In vaccinated SOT recipients even after full vaccination, there is a reduction of the risk of mortality, but the course of COVID-19 may continue to be severe, influenced by the time from transplant, the net state of immunosuppression and having suffered graft rejection or dysfunction. SOT recipients develop lower immunity from mRNA vaccines with suboptimal response. Treatment with mAbs provides favorable outcomes in non-hospitalized SOT recipients at high risk for severe disease, with lower rates of hospitalization, emergency department visits, ICU care, progression to severe disease, and death. However, broad vaccination and therapeutic options are required, particularly in light of the tendency of the SARS-CoV-2 virus to adapt and evade both natural

Los receptores de trasplantes de órganos sólidos (TOS) presentan un alto riesgo de infección por el virus SARS-CoV-2 debido al tratamiento inmunosupresor y múltiples comorbilidades. La COVID-19 puede ser potencialmente mortal en receptores de TOS, con un aumento de la probabilidad de progresión a enfermedad grave. Este trabajo presenta una revisión actualizada del impacto de la COVID-19 en receptores de TOS. En los receptores de TOS no vacunados, la COVID-19 se asocia con una alta tasa de mortalidad, hospitalización, ingreso en la UCI y deterioro del injerto o rechazo. En los pacientes vacunados, incluso con pauta de vacunación completa, se reduce el riesgo de mortalidad, pero el curso de la COVID-19 puede continuar siendo grave en función del tiempo desde el trasplante, el estado neto de inmunosupresión y haber sufrido rechazo o disfunción del injerto. Los receptores de TOS presentan una baja inmunogenicidad a las vacunas de ARNm y respuesta subóptima. El tratamiento con anticuerpos monoclonales (AMC) en receptores de TOS no hospitalizados con alto riesgo de enfermedad grave, se asocia con menores tasas de hospitalización, visitas a urgencias, ingreso en UCI, progresión a enfermedad grave y muerte. Sin embargo, se requieren nuevas vacunas y opciones terapéuticas, teniendo en cuenta la tendencia del virus SARS-CoV-2 a adaptarse y a evadir tanto la inmunidad natural como la inducida por la vacuna (Au)and vaccine-induced immunity (AU)

Lower serum expression of miR-181c-5p is associated with increased plasma levels of amyloid-beta 1-40 and cerebral vulnerability in normal aging.

BACKGROUND: Previous studies have shown that expression levels of miR-181c are downregulated by amyloid-ß (Aß) deposition and chronic cerebral hypoperfusion, both factors largely associated with the development of AD. Moreover, reduced 2-[18F]fluoro-2-deoxy-D-glucose (FDG)-PET brain metabolism and volume loss of regions of the medial temporal lobe have been generally recognized as hallmarks of AD. Based on this evidence, we have here investigated potential associations between serum levels of miR-181c-5p and these AD signatures in asymptomatic elderly subjects. METHODS: Ninety-five normal elderly subjects underwent clinical, cognitive, structural MRI, and FDG-PET explorations. Serum expression levels of miR-181c-5p and plasma Aß concentrations were further analyzed in this cohort. Regression analyses were performed to assess associations between serum miR-181c-5p levels and cognitive functioning, plasma Aß, structural and metabolic brain changes. RESULTS: Decreased serum expression of miR-181c-5p was associated with increased plasma levels of Aß1-40, deficits in cortical glucose metabolism, and volume reduction of the entorhinal cortex. No significant associations were found between lower miR-181c-5p levels and cognitive deficits or cortical thinning. CONCLUSIONS: These findings suggest that deregulation of serum miR-181c-5p may indicate cerebral vulnerability in late life.