G. Rosso scite author profile

Ischemia/reperfusion injury is an unavoidable relevant consequence after kidney transplantation and influences short term as well as long-term graft outcome. Clinically ischemia/reperfusion injury is associated with delayed graft function, graft rejection, chronic rejection and chronic graft dysfunction. Ischemia/reperfusion affects many regulatory systems at the cellular level as well as in the renal tissue that result in a distinct inflammatory reaction of the kidney graft. Underlying factors of ischemia reperfusion include energy metabolism, cellular changes of the mitochondria and cellular membranes, initiation of different forms of cell death-like apoptosis and necrosis together with a recently discovered mixed form termed necroptosis. Chemokines and cytokines together with other factors promote the inflammatory response leading to activation of the innate immune system as well as the adaptive immune system. If the inflammatory reaction continues within the graft tissue, a progressive interstitial fibrosis develops that impacts long-term graft outcome. It is of particular importance in kidney transplantation to understand the underlying mechanisms and effects of ischemia/reperfusion on the graft as this knowledge also opens strategies to prevent or treat ischemia/reperfusion injury after transplantation in order to improve graft outcome.

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Good outcomes with Cyclosporine very low exposure with Everolimus high exposure in renal transplant patients

Bertoni¹,

Larti²,

Rosso³

et al. 2011

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Reclassification of membranoproliferative glomerulonephritis: Identification of a new GN: C3GN

Salvadori¹,

Rosso²

2016

WJN

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This review revises the reclassification of the membranoproliferative glomerulonephritis (MPGN) after the consensus conference that by 2015 reclassified all the glomerulonephritis basing on etiology and pathogenesis, instead of the histomorphological aspects. After reclassification, two types of MPGN are to date recognized: The immunocomplexes mediated MPGN and the complement mediated MPGN. The latter type is more extensively described in the review either because several of these entities are completely new or because the improved knowledge of the complement cascade allowed for new diagnostic and therapeutic approaches. Overall the complement mediated MPGN are related to acquired or genetic cause. The presence of circulating auto antibodies is the principal acquired cause. Genetic wide association studies and family studies allowed to recognize genetic mutations of different types as causes of the complement dysregulation. The complement cascade is a complex phenomenon and activating factors and regulating factors should be distinguished. Genetic mutations causing abnormalities either in activating or in regulating factors have been described. The diagnosis of the complement mediated MPGN requires a complete study of all these different complement factors. As a consequence, new therapeutic approaches are becoming available. Indeed, in addition to a nonspecific treatment and to the immunosuppression that has the aim to block the auto antibodies production, the specific inhibition of complement activation is relatively new and may act either blocking the C5 convertase or the C3 convertase. The drugs acting on C3 convertase are still in different phases of clinical development and might represent drugs for the future. Overall the authors consider that one of the principal problems in finding new types of drugs are both the rarity of the disease and the consequent poor interest in the marketing and the lack of large international cooperative studies.

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Subcutaneous Nodules and Infectious Complications in Renal Allograft Recipients

Caroti

Zanazzi

Rogasi

et al. 2010

Transplantation Proceedings

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Chronic Kidney Disease Is Still Present After Renal Transplantation With Excellent Function

Bertoni

Rosati

Larti

et al. 2006

Transplantation Proceedings

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G. Rosso

Update on ischemia-reperfusion injury in kidney transplantation: Pathogenesis and treatment

Good outcomes with Cyclosporine very low exposure with Everolimus high exposure in renal transplant patients

Reclassification of membranoproliferative glomerulonephritis: Identification of a new GN: C3GN

Subcutaneous Nodules and Infectious Complications in Renal Allograft Recipients

Chronic Kidney Disease Is Still Present After Renal Transplantation With Excellent Function

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