Helena Sá
University of Coimbra
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International Reviews of Immunology | 2017
Helena Sá; Rita Leal; Manuel Santos Rosa
To deride the hope of progress is the ultimate fatuity, the last word in poverty of spirit and meanness of mind. There is no need to be dismayed by the fact that we cannot yet envisage a definitive solution of our problems, a resting-place beyond which we need not try to go. —P.B. Medawar, 1969* Thomas E. Starlz, also known as the Father of Clinical Transplantation, once said that organ transplantation was the supreme exception to the rule that most major advances in medicine spring from discoveries in basic science [Starzl T. The mystique of organ transplantation. J Am Coll Surg 2005 Aug;201(2):160–170]. In fact, the first successful identical-twin kidney transplantation performed by Murrays team in December 1954 (Murray J et al. Renal homotransplantations in identical twins. Surg Forum 1955;6:432–436) was the example of an upside down translation medicine: Human clinical transplantation began and researchers tried to understand the underlying immune response and how to control the powerful rejection pathways through experimental models. In the last 20 years, we have witnessed an amazing progress in the knowledge of immunological mechanisms regarding alloimmune response and an outstanding evolution on the identification and characterization of major and minor histocompatibility antigens. This review presents an historical and clinical perspective of those important advances in kidney transplantation immunology in the last 20 years, which contributed to the improvement in patients’ quality of life and the survival of end-stage renal patients. In spite of these significant progresses, some areas still need substantial progress, such as the definition of non-invasive biomarkers for acute rejection; the continuous reduction of immunosuppression; the extension of graft survival, and finally the achievement of real graft tolerance extended to HLA mismatch donor: recipient pairs.
Case Reports | 2016
Brigite Aguiar Cardoso; Rita Leal; Helena Sá; Mário Campos
AL amyloidosis is a clonal plasma cell proliferative disorder characterised by extracellular tissue deposits of insoluble fibrils derived from κ or λ immunoglobulin light chains. The most common organs affected by AL amyloidosis are the kidney, presenting with nephrotic syndrome and/or progressive renal dysfunction, and the heart, with restrictive cardiomyopathy. Hepatic deposition of fibrils occurs in half the cases but the liver is rarely the predominantly affected organ. The most common presentation of hepatic amyloidosis is hepatomegaly with elevated alkaline phosphatase. Acute liver failure with cholestasis and jaundice is a rare complication, with a prevalence of approximately 5%, and is usually associated with a worse prognosis. We report a case of a 39-year-old man admitted to our nephrology department with an unusual presentation of primary amyloidosis with nephrotic syndrome and acute liver failure, complicated by obstructive cholestasis resulting in death 2 months after diagnosis.
F1000Research | 2016
Rita Leal; José Simplício; Ana Galvão; Paulo Santos; Helena Sá; Mário Campos; Manuel Santos Rosa
Archive | 2015
Luís Rodrigues; Fernando Macário; Cátia Pego; Marta Neves; Catarina Romãozinho; Lídia Santos; Rui Alves; Helena Sá; Alfredo Mota; Mário Campos
Archive | 2014
Marta Neves; Luís Rodrigues; Helena Sá; Jorge Pratas; Mário Campos
Archive | 2014
Luís Rodrigues; Brigite Aguiar; Marta Neves; Tânia Santos; Telma Santos; José Gago; Helena Sá; Mário Campos; Carol Marinho
Archive | 2009
Flora Rico Sofia; Helena Sá; Jorge Pratas; Henrique Gomes; Mário Campos
Archive | 2007
Flora Rico Sofia; Helena Sá; Luís Freitas; Henrique Gomes; Mário Campos
Revista Portuguesa de Nefrolologia e Hipertensão | 2006
Helena Sá; Vera Alves; Filomena Oliveira; Anabela Mota-Pinto; Mário Campos; Manuel Santos-Rosa
Cytometry Supplement | 2000
Helena Sá; Vera Alves; Filomena Oliveira; Adelino Marques; Mário Campos; Manuel Santos Rosa