Silvia Arienti
University of Padua
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Autoimmunity Reviews | 2008
Andrea Doria; Silvia Arienti; Mariaelisa Rampudda; M Canova; M Tonon; Piercalo Sarzi-Puttini
Despite the improvement of systemic lupus erythematosus (SLE) survival observed in the last decades, the long-term prognosis of these patients remains poor mainly due to complications of the disease and/or of its treatment. Therefore, in order to improve SLE prognosis, we should try to avoid long-term complications by adopting, early in the disease course, some strategies directed to prevent infections, atherosclerosis and cancer. Moreover, since it has been shown that autoantibodies appear before clinical manifestations in SLE, the question of whether or not asymptomatic individuals with a reliable positive serology should be treated arises. Other than advising these individuals to avoid sun exposure, drugs implicated in drug-induced lupus and cigarette smoking, the use of vitamin D and hydroxychloroquine could be considered. Finally, early SLE diagnosis has led to a modification of disease clinical spectrum at disease onset with an increased frequency of mild disease manifestations over severe ones. Thus great effort should be made in order to identify early in the disease course risk factors for the development of severe SLE manifestations. Finally patients with mild disease carrying factors predictive of severe manifestations should be treated more aggressively than we have done up to now.
Annals of the New York Academy of Sciences | 2006
Andrea Doria; Luca Iaccarino; Piercarlo Sarzi-Puttini; Anna Ghirardello; Sandra Zampieri; Silvia Arienti; Maurizio Cutolo; Silvano Todesco
Abstract: Successful pregnancy depends on an adaptation of the maternal immune system that becomes tolerant to fetal antigens of paternal origin. The altered immune regulation induced by pregnancy occurs predominantly at the maternal–fetal interface, but it has also been observed in the maternal circulation. Th1/Th2 shift is one of the most important immunologic changes during gestation. It is due to the progressive increase of estrogens, which reach peak level in the third trimester of pregnancy. At these high levels, estrogens suppress the Th1‐mediated responses and stimulate Th2‐mediated immunologic responses. For this reason Th1‐mediated diseases, such as rheumatoid arthritis, tend to improve, while Th2‐mediated diseases, such as systemic lupus erythematosus (SLE) tend to worsen during pregnancy. However, in some recent studies SLE flare‐ups were less frequently observed in the third trimester of gestation in comparison to the second trimester and postpartum period. These data are apparently in contrast to the Th2 immune‐response polarization expected during pregnancy due to the progressive increase of estrogens. Some further data suggest that in SLE patients estradiol serum levels are surprisingly lower than expected during the third trimester of pregnancy, probably due to a placental compromise. This occurrence could lead to a lower‐than‐expected increase of IL‐6, accounting for the low humoral immune response and the low disease activity observed in the third trimester of pregnancy in such patients.
Annals of the New York Academy of Sciences | 2005
Sandra Zampieri; Luca Iaccarino; Anna Ghirardello; Elena Tarricone; Silvia Arienti; Piercarlo Sarzi-Puttini; Pierfranca Gambari; Andrea Doria
Abstract: Over the past number of years numerous data have been published regarding increased atherosclerosis in patients with systemic lupus erythematosus (SLE), and it has been shown that premature or accelerated atherosclerosis is an important cause of morbidity and mortality in these patients. Besides the traditional risk factors for cardiovascular disease, the association between SLE and atherosclerosis can be attributed to additional risk factors closely related to inflammation and autoimmunity. In particular, several autoantibodies and their respective autoantigens have been identified as possible factors in the development and progression of the atherosclerotic process in SLE. The understanding of SLE‐related risk factors for enhanced atherosclerosis could shed more light on disease mechanisms, leading to new therapeutic strategies for the treatment of cardiovascular diseases in SLE patients. In the present paper, the biological characteristics and possible pathogenetic role of the oxidized low‐density lipoprotein (oxLDL) and anti‐oxLDL, β2‐glycoprotein I (β2GPI) and anti‐β2GPI, and heat‐shock protein 60/65 (HSP60/65) and anti‐HSP60/65 autoantibody systems are summarized.
Autoimmunity | 2006
Sandra Zampieri; Anna Ghirardello; Luca Iaccarino; Chiara Briani; Piercarlo Sarzi-Puttini; Fabiola Atzeni; Silvia Arienti; Silvano Todesco; Andrea Doria
In genetically predisposed individuals, viruses, bacteria, or parasitic infectious agents are suspected to induce autoimmunity and/or to exacerbate the disease once the self-tolerance is broken. Although direct evidence for this association is still lacking, numerous data from animal models as well as from humans support the hypothesis of a direct contribution of pathogens to the induction of several autoimmune diseases. This review focused on the possible role of infectious agents as triggers of autoimmunity in polymyositis (PM) and dermatomyositis (DM). Epidemiological studies, clinical and experimental findings that support the hypothesis of infection-induced PM and DM are summarized and discussed. In addition, immune response abnormalities and immunosuppressive medications may be responsible for the high percentage of infectious complications in PM and DM patients. In this review, the increased risk of developing infections in these patients is also underlined and published data are reported.
Annals of the New York Academy of Sciences | 2007
Luca Iaccarino; Silvia Arienti; Mariaelisa Rampudda; M Canova; Fabiola Atzeni; Piercarlo Sarzi Puttini; Andrea Doria
Abstract: Mycophenolate mofetil (MMF) is an immunosuppressive agent initially used in the treatment of transplant recipients. MMF has been used in renal, heart, and liver transplantation, where it seems more effective than other immunosuppressive regimens in reducing the incidence of acute rejection episodes. MMF has a variety of immunosuppressive effects, including selective suppression of T and B lymphocyte proliferation, and has been more recently used in many autoimmune inflammatory conditions. Systemic lupus erythematosus (SLE) is an autoimmune disease that can potentially involve any organ or system of the human body. Glomerulonephritis (GLN) has been recognized as the most frequent severe manifestation of SLE, leading to poor long‐term prognosis. In the treatment of lupus GLN, several therapeutic approaches, all including immunosuppressive drugs, such as cyclophosphamide, azathioprine, or cyclosporine A, have been used. The short‐ and long‐term toxicity of these drugs limits their use in a substantial number of patients. Over the last few years, MMF has emerged as an alternative therapeutic regimen in lupus GLN, mainly for patients refractory to other therapies. These studies have shown that it is highly effective and generally well tolerated.
Reproductive Toxicology | 2006
Andrea Doria; Luca Iaccarino; Silvia Arienti; Anna Ghirardello; Sandra Zampieri; Maria Elisa Rampudda; Maurizio Cutolo; Angela Tincani; Silvano Todesco
Zeitschrift Fur Rheumatologie | 2006
Andrea Doria; Luca Iaccarino; Anna Ghirardello; Silvia Arienti; Sandra Zampieri; Me Rampudda; Angela Tincani; Silvano Todesco
Zeitschrift Fur Rheumatologie | 2006
Andrea Doria; Luca Iaccarino; Anna Ghirardello; Silvia Arienti; Sandra Zampieri; Me Rampudda; Angela Tincani; Silvano Todesco
Zeitschrift Fur Rheumatologie | 2006
Andrea Doria; Luca Iaccarino; Anna Ghirardello; Silvia Arienti; Sandra Zampieri; Me Rampudda; Angela Tincani; Silvano Todesco
/data/revues/00029343/v119i8/S0002934306001938/ | 2011
Andrea Doria; Luca Iaccarino; Anna Ghirardello; Sandra Zampieri; Silvia Arienti; Piercarlo Sarzi-Puttini; Fabiola Atzeni; Antonio Piccoli; Silvano Todesco