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Featured researches published by Alberto Baraldi.


Nephron | 1996

No Direct Evidence of Increased Lipid Peroxidation in Hemodialysis Patients

Sebastiano Banni; Leonardo Lucchi; Alberto Baraldi; Barbara Botti; Gianni Cappelli; Francesco P. Corongiu; Maria Assunta Dessì; Aldo Tomasi; Egidio Lusvarghi

Lipid peroxidation, as measured by the thiobarbituric acid test, has been reported to have increased in hemodialysis (HD) patients, even though the test has low specificity in vivo. Conjugated diene fatty acid (CDFA) hydroperoxides are formed during lipid peroxidation, but not all conjugated dienes (CD) detected in humans originate from lipid peroxidation: octadeca-9,11-dienoic acid, a nonhydroperoxide CD derivative of linoleic acid (CDLA), has a dietary origin. We evaluated CDFA hydroperoxides, CDLA and linoleic acid, using high-performance liquid chromatography, in lipids extracted from plasma, adipose tissue and RBC membranes obtained from 25 patients treated with HD, 16 patients treated with hemodiafiltration (HDF) and 29 controls. No differences in the levels of CDFA hydroperoxides and linoleic acid were seen in any of the groups. Concentrations of CDLA were found to be significantly high in the adipose tissue and low in the RBC membranes of HD patients. HDF-treated patients showed the same results as HD patients. No direct evidence of increased lipid peroxidation was found in HD patients. This does not exclude the possibility that lipid peroxidation is increased and escapes direct detection due to the bodys homeostatic control eliminating the increased production of hydroperoxides. Both HD- and HDF-treated patients showed a significant change in CDLA concentrations, either in the adipose tissue, or in the RBC membranes. These dietary CD may be mistaken for markers of lipid peroxidation by conventional methodologies.


Nephron | 1992

Very late activation-3 integrin is the dominant β1-integrin on the glomerular capillary wall : an immunofluorescence study in nephrotic syndrome

Alberto Baraldi; Luciana Furci; Giovanna Zambruno; Elisabetta Rubbiani; Giorgio Annessi; Egidio Lusvarghi

The expression of alpha 2; alpha 3; alpha 5; alpha 6-subunits of the beta 1 [very late activation (VLA)] integrin family was studied in kidney specimens using an immunofluorescent technique. 6 specimens from normal kidney were compared with 10 specimens from patients affected by various glomerulopathies [minimal change nephropathy (MCN), membranous nephropathy (MN) and systemic lupus erythematosus nephritis (SLEN)]. On normal glomeruli, alpha 3 was the dominant integrin, being mainly present on podocytes and showing a linear fluorescent pattern codistributed with laminin. In MCN and SLEN, alpha 3 presented a normal pattern. In MN, alpha 3 revealed a trabecular picture on thickened glomerular basement membranes. Moreover, in stage-III MN, a segmental loss of alpha 3-integrin was detected. In our opinion, VLA-3 may offer an interesting approach to the study of the relationships between podocytes and their substrate.


Nephron | 1994

Beta-1 Integrins in the Normal Human Glomerular Capillary Wall: An Immunoelectron Microscopy Study

Alberto Baraldi; Giovanna Zambruno; Luciana Furci; V. Manca; C. Vaschieri; Egidio Lusvarghi

The localization of the alpha 2, alpha 3 and alpha 6 subunits of the beta 1 integrin family on different cells of the glomerular capillary wall and on juxta-capillary mesangium was investigated using an immunoelectron microscopic technique on freshly harvested normal human glomeruli. Alpha 2 beta 1, alpha 3 beta 1 and alpha 6 beta 1 were weakly expressed on both luminal and abluminal surfaces of glomerular endothelial cells; alpha 2 beta 1 and alpha 3 beta 1 were also found on the mesangium of the juxta-capillary areas. Alpha 3 beta 1 was regularly present in great density on the basal and lateral surface of podocyte foot processes, confirming alpha 3 beta 1 as the unique beta 1 integrin on glomerular epithelial cells. None of these integrins was strictly polarized along the glomerular basement membrane, thus suggesting, in agreement with recent literature, that these molecules perform other biological functions in addition to adhesivity.


Nephrology Dialysis Transplantation | 2014

A clinical stratification tool for chronic kidney disease progression rate based on classification tree analysis

Paola Rucci; Marcora Mandreoli; Dino Gibertoni; Alessandro Zuccalà; Maria Pia Fantini; Jacopo Lenzi; Antonio Santoro; Roberto Scarpioni; Sara De Amicis; Carlo Buzio; Salvatore David; Sonia Pasquali; Mattia Corradini; Gianni Cappelli; Fabio Olmeda; Alberto Baraldi; Francesco Caruso; Sergio Stefoni; Claudio Orsi; Cecilia Cannarile; Pierpaolo Di Nicolò; Alda Storari; Giorgia Russo; A. Buscaroli; Mattia Monti; Giovanni Mosconi; Stefania Cristino; Carlo Feletti; Leopoldo Baldrati; Angelo Rigotti

BACKGROUND Registry-based studies have identified risk factors for chronic kidney disease (CKD) and for progression to end-stage renal disease. However, usually, these studies do not incorporate sequential measurements of kidney function and provide little information on the prognosis of individual patients. The aim of this study is to identify which combinations of demographic and clinical characteristics are useful to discriminate patients with a differential annual decline in glomerular filtration rate (GFR). METHODS This observational retrospective study includes patients enlisted in the registry of the Prevention of Progressive Renal Insufficiency Project of Emilia-Romagna region (Italy) from July 2004 to June 2010, with at least four serum creatinine measurements. Classification tree analysis (CTA) was used to identify subgroups of patients with a different annual GFR decline using demographic and laboratory data collected at study entry. RESULTS The CTA procedure generated seven mutually exclusive groups. Among patients with proteinuria, those with a baseline estimated GFR (eGFR) of >33 mL/min/1.73 m(2) exhibited the fastest illness progression in the study population (-3.655 mL/min/1.73 m(2)), followed by patients with a baseline eGFR of <33 mL/min/1.73 m(2) and a baseline serum phosphorus of >4.3 mg/dL (-2.833 mL/min/1.73 m(2)). Among patients without proteinuria, those aged <67 years exhibited a significantly faster progression, which was even faster for the subgroup with diabetes. Among patients aged >67 years, females had on average a stable eGFR over time, with a large variability. CONCLUSIONS It is possible to rely on a few variables typically accessible in routine clinical practice to stratify patients with a different CKD progression rate. Stratification can be used to guide decisions about the follow-up schedule, treatments to slow progression of kidney disease, prevent its complications and to begin planning for dialysis and transplantation.


Nephron | 1996

Influence of Urinary Calcium Concentration on Erythrocyte Morphology

Decenzio Bonucchi; Marco Ballestri; Federica Bettelli; Alberto Baraldi; Mauro Gola; Leonardo Lucchi; Egidio Lusvarghi

The effect of the urinary calcium concentration (CaU) on erythrocyte morphology was studied by incubating erythrocytes in urine with prefixed CaUs of 5, 10, 20 and 40 mmol/l by addition of CaCl2. The same experiment was carried out on erythrocytes preincubated with levo-verapamil (l-V) at 10, 100 and 200 mumol/l. Phase contrast microscopy observations were performed at 0, 30, 60, 120, and 240 min by 2 experienced investigators. At 0 min the erythrocytes showed a clear extraglomerular pattern. At 60 min marked morphological and volumetric alterations were evident when the CaU was > or = 10 mmol/l. On the contrary, no change was found when red cells were treated with > or = 100 mumol/l l-V, independent of the CaU. Dysmorphic erythrocyturia has been related to transglomerular passage even if it was sporadically observed in hypercalciuric or lithiasic patients. This work suggests a role for a high CaU in causing the formation of microcytic and warped erythrocytes. In our opinion, in hypercalciuric urine the appearance of dysmorphic or mixed hematuria does not necessarily indicate transglomerular passage.


Nephrology Dialysis Transplantation | 1998

Acute renal failure of medical type in an elderly population

Alberto Baraldi; Marco Ballestri; R Rapanà; L. Lucchi; Paola Borella; M Leonelli; Luciana Furci; Egidio Lusvarghi


Gastroenterology | 2001

Liver and Kidney Foreign Bodies Granulomatosis in a Patient With Malocclusion, Bruxism, and Worn Dental Prostheses

Marco Ballestri; Alberto Baraldi; Antonietta M. Gatti; Luciana Furci; Alberto Bagni; Paola Loria; Renato Rapanà; Nicola Carulli; Alberto Albertazzi


Nephrology Dialysis Transplantation | 1995

β1 and β3 integrin upregulation in rapidly progressive glomerulonephritis

Alberto Baraldi; G. Zambruno; Luciana Furci; Marco Ballestri; A. Tombesi; D. Ottani; L. Lucchi; Egidio Lusvarghi


Nephrology Dialysis Transplantation | 1998

Vascular access for haemodialysis: from surgical procedure to an integrated therapeutic approach.

Decenzio Bonucchi; A D'Amelio; M. Grosoli; Alberto Baraldi; Gianni Cappelli


Nephron | 1996

Contents, Vol. 74, 1996

R.P. Woitas; T. Morioka; P. Dionisio; E. Stramignoni; G. Passarino; A. Pucci; M. Valenti; I.M. Berto; M. Portigliatti Barbos; A. Cadario; G. Gasparri; P. Bajardi; Charles J. Diskin; Thomas J. Stokes; Leslie W. Panus; Kuddusi Cengiz; Esin Özyilkan; Arif Mansur Coşar; Murat Gunaydin; Akio Inui; Hideaki Inoue; Masaharu Uemoto; Masato Kasuga; Hiroshi Taniguchi; Y. Hori; J.G. van den Berg; M.G. Koopman; L. Arisz; Tadasu Ikeda; Tazue Hoshino

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Egidio Lusvarghi

University of Modena and Reggio Emilia

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Luciana Furci

University of Modena and Reggio Emilia

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Marco Ballestri

University of Modena and Reggio Emilia

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Gianni Cappelli

University of Modena and Reggio Emilia

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Leonardo Lucchi

University of Modena and Reggio Emilia

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