Your search keyword '"Abelli, Massimo"' showing total 2 results

1. Impediments to Heart Transplantation in Adults With MELASMT-TL1:m.3243A>G Cardiomyopathy.

Author

Di Toro, Alessandro, Urtis, Mario, Narula, Nupoor, Giuliani, Lorenzo, Grasso, Maurizia, Pasotti, Michele, Pellegrini, Carlo, Serio, Alessandra, Pilotto, Andrea, Antoniazzi, Elena, Rampino, Teresa, Magrassi, Lorenzo, Valentini, Adele, Cavallini, Anna, Scelsi, Laura, Ghio, Stefano, Abelli, Massimo, Olivotto, Iacopo, Porcu, Maurizio, and Gavazzi, Antonello

Subjects

*MELAS syndrome, *HEART transplantation, *CARDIOMYOPATHIES, *MITOCHONDRIAL DNA, *CHRONIC kidney failure, *HEARING disorders, *MUSCLE diseases, *DNA, *GENETIC mutation, *MITOCHONDRIAL encephalomyopathies, *DISEASE complications, CHRONIC kidney failure complications

Abstract

Background: The heart is commonly involved in maternally inherited mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes (MELAS) syndrome caused by the MT-TL1 m.3243A>G mutation of the mitochondrial DNA. Heart transplantation (HTx) is controversial and has rarely been performed with conflicting results.Objectives: We analyzed factors preventing HTx in consecutive adult patients with MELASMT-TL1:m.3243A>G cardiomyopathy diagnosed and followed during the last 23 years in our HTx referral center.Methods: The series consists of 14 unrelated adult probands who were referred for evaluation of cardiomyopathy from 1998 to 2021. None had a suspected diagnosis of MELAS before referral. All patients underwent clinical and genetic visit and counseling, mitochondrial DNA sequencing, cardiovascular investigation (including right heart catheterization and endomyocardial biopsy in 10), multidisciplinary assessment, and biochemical tests. Family screening identified 2 affected relatives.Results: The cardiac phenotype was characterized by hypertrophic, concentric, nonobstructive cardiomyopathy that often evolved into a dilated cardiomyopathy-like phenotype. Of the 14 probands, 7 were potential candidates for HTx, 2 for heart and kidney Tx, and 1 was on the active HTx list for 3 years. None of the 10 probands underwent HTx. One is currently being evaluated for HTx. All had diabetes, hearing loss, and myopathy, and 10 had chronic kidney disease and progressive encephalomyopathy. During follow-up, 10 died from heart failure associated with multiorgan failure within 5 years of the genetic diagnosis.Conclusions: High risk of stroke-like episodes, chronic kidney disease, and wasting myopathy in MELASMT-TL1:m.3243A>G patients prevents activation of plans for HTx. As a result, the management of their cardiomyopathy in this syndromic context remains an unmet clinical need. [ABSTRACT FROM AUTHOR]

Published

2022

2. Sirolimus vs cyclosporine after induction with basiliximab does not promote regulatory T cell expansion in de novo kidney transplantation: Results from a single-center randomized trial.

Author

Libetta, Carmelo, Esposito, Pasquale, Gregorini, Marilena, Margiotta, Elisa, Martinelli, Claudia, Borettaz, Ilaria, Canevari, Michele, Rampino, Teresa, Ticozzelli, Elena, Abelli, Massimo, Meloni, Federica, and Dal Canton, Antonio

Subjects

*RAPAMYCIN, *CYCLOSPORINE, *BASILIXIMAB, *T cells, *KIDNEY transplant patients, *IMMUNOCOMPETENT cells, *IMMUNOSUPPRESSION

Abstract

Regulatory T cells (Tregs), defined as CD4 + CD25 + highFoxP3 + CD127 − cells, could promote tolerance in renal transplantation (Tx). In an open-label, randomized, controlled trial 62 de-novo Tx recipients received induction with basiliximab and cyclosporine A (CsA) for the first month after Tx and then were assigned to treatment with sirolimus (SRL) or CsA and followed up for 2 years. The primary endpoint was to evaluate the effects of induction and maintenance treatments on circulating Tregs, while the secondary endpoint was the assessment of Treg renal infiltration and the relationship between Treg count and clinical outcomes. There were no significant differences in either circulating or tissue Treg number between the two groups. At 1 month post-Tx, all patients presented a profound Treg depletion, followed by a significant increase in Tregs that resulted stable during the follow-up. The same trend was also observed for non-activated Tregs (CD69 −) and for other immunocompetent cells (CD4 + and CD8 + T cells, B cells and NK cells). Moreover, the Treg count did not correlate either with renal function or with acute rejection and graft loss. Initial immunosuppression is crucial to regulate circulating Tregs, regardless of subsequent immunosuppressive maintenance regimens. Strategies aiming to promote tolerance should consider the effects of different induction regimens. [ABSTRACT FROM AUTHOR]

Published

2015