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2. Evidence for charge-based mimicry in anti dsDNA antibody generation

Author

Maurizio Bruschi, Andrea Angeletti, Xhuliana Kajana, Gabriella Moroni, Renato Alberto Sinico, Micaela Fredi, Augusto Vaglio, Lorenzo Cavagna, Federico Pratesi, Paola Migliorini, Francesco Locatelli, Giulia Pazzola, Giampaola Pesce, Marcello Bagnasco, Angelo Manfredi, Giuseppe Alvise Ramirez, Pasquale Esposito, Simone Negrini, Federica Bui, Barbara Trezzi, Giacomo Emmi, Ilaria Cavazzana, Valentina Binda, Paride Fenaroli, Isabella Pisani, Carlomaurizio Montecucco, Domenico Santoro, Francesco Scolari, Stefano Volpi, Marta Mosca, Angela Tincani, Giovanni Candiano, Enrico Verrina, Franco Franceschini, Angelo Ravelli, Marco Prunotto, Pier Luigi Meroni, Gian Marco Ghiggeri, Bruschi, M, Angeletti, A, Kajana, X, Moroni, G, Sinico, R, Fredi, M, Vaglio, A, Cavagna, L, Pratesi, F, Migliorini, P, Locatelli, F, Pazzola, G, Pesce, G, Bagnasco, M, Manfredi, A, Ramirez, G, Esposito, P, Negrini, S, Bui, F, Trezzi, B, Emmi, G, Cavazzana, I, Binda, V, Fenaroli, P, Pisani, I, Montecucco, C, Santoro, D, Scolari, F, Volpi, S, Mosca, M, Tincani, A, Candiano, G, Verrina, E, Franceschini, F, Ravelli, A, Prunotto, M, Meroni, P, and Ghiggeri, G

Subjects
Immunology, IgG2, DNA, anti-dsDNA antibodie, Lupus Nephritis, Anionic epitope, Antibodies, Antinuclear, Immunoglobulin G, Immunology and Allergy, Humans, Lupus Erythematosus, Systemic, Mimicry, anti-Annexin A1 antibodie, Isotype, Autoantibodies, Annexin A1
Abstract

Mechanisms for the generation of anti-dsDNA autoantibodies are still not completely elucidated. One theory states that dsDNA interacts for mimicry with antibodies raised versus other antigens but molecular features for mimicry are unknown. Here we show that, at physiological acid-base balance, anti-Annexin A1 binds IgG2 dsDNA in a competitive and dose-dependent way with Annexin A1 and that the competition between the two molecules is null at pH 9. On the other hand, these findings also show that dsDNA and Annexin A1 interact with their respective antibodies on a strictly pH-dependent basis: in both cases, the binding was minimal at pH 4 and maximal at pH9-10. The anionic charge of dsDNA is mainly conferred by the numerous phosphatidic residues. The epitope binding site of Annexin A1 for anti-Annexin A1 IgG2 was here characterized as a string of 34 amino acids at the NH2 terminus, 10 of which are anionic. Circulating levels of anti-dsDNA and anti-Annexin A1 IgG2 antibodies were strongly correlated in patients with systemic lupus erythematosus (n 496) and lupus nephritis (n 425) stratified for age, sex, etc. These results show that dsDNA competes with Annexin A1 for the binding with anti-Annexin A1 IgG2 on a dose and charged mediated base, being able to display an inhibition up to 75%. This study provides the first demonstration that dsDNA may interact with antibodies raised versus other anionic molecules (anti-Annexin A1 IgG2) because of charge mimicry and this interaction may contribute to anti-dsDNA antibodies generation.

Published
2022

3. Long-term kidney outcome of patients with rheumatological diseases and antineutrophil cytoplasmic antibody-glomerulonephritis: comparison with a primitive ANCA-glomerulonephritis cohort

Author

Laura, Locatelli, Marta, Calatroni, Francesco, Reggiani, Grazia Dea, Bonelli, Maria, Gerosa, Lorenza Maria, Argolini, Barbara, Trezzi, Nicoletta, Del Papa, Claudio, Angelini, Maria Rosa, Pozzi, Renato Alberto, Sinico, and Gabriella, Moroni

Subjects
Rheumatology, Immunology, Immunology and Allergy
Abstract

Antineutrophil cytoplasmic antibody (ANCA) may appear in the course of rheumatic diseases (RD) but the kidney involvement is very rare and the prognosis poorly defined.We retrospectively identified patients with RD among 153 patients with ANCA glomerulonephritis (ANCA-GN). Their clinical/histological presentation and outcome were compared with that of primitive ANCA-GN patients (1:4) matched for sex, age, ANCA type and follow-up.Nine patients (5.9%) were included: three had rheumatoid arthritis, two systemic sclerosis, two psoriatic arthritis, one ankylosing spondylitis and one seronegative spondylarthritis. Seven patients were MPO positive, two PR3 positive. ANCA-GN developed 74 months after RD with microscopic haematuria and acute kidney dysfunction in all but two patients. After 68-month follow-up, four patients (44.4%) achieved response to therapy defined as eGFR60/min/1,73 m2 or stable, no microscopic haematuria and negative ANCA. At ANCA-GN diagnosis, serum creatinine and C-reactive protein were significantly lower in RD-ANCA-GN (2.38 vs. 3.34mg/dl, p=0.05 and 2.3mg/dl vs. 7.2mg/dl; p=0.05, respectively) while haemoglobin was higher (12.3g/dl vs. 9.3g/dl p0.01) than in the 36 primitive ANCA-GN patients of control group. At kidney biopsy, focal forms were more frequent in RD patients (44.45% vs. 18.75%, p=0.11). The treatment between the two groups was not significantly different. At last observation, the percentage of patients with ESKD was lower in RD than in controls (11.1%vs. 30.5%; p=0.23).Patients with RD seem to develop ANCA-GN with less severe clinical/histological kidney involvement, and better long-term kidney survival than primitive ANCA-GN. This is probably due to the strict monitoring of RD patients that allows a prompter ANCA-GN diagnosis and treatment.

Published
2022

4. Belimumab may decrease flare rate and allow glucocorticoid withdrawal in lupus nephritis (including dialysis and transplanted patient)

Author

Piergiorgio Messa, Maria Rosa Pozzi, Nicoletta Del Papa, Giulia Porata, Giulia Frontini, Gabriella Moroni, Paolo Fabbrini, Barbara Trezzi, Renato Alberto Sinico, Valentina Binda, Lorenzo Beretta, Binda, V, Trezzi, B, Del Papa, N, Beretta, L, Frontini, G, Porata, G, Fabbrini, P, Pozzi, M, Messa, P, Sinico, R, and Moroni, G

Subjects
Nephrology, medicine.medical_specialty, medicine.medical_treatment, SLE, 030232 urology & nephrology, Lupus nephritis, Systemic lupus erythematosu, 030204 cardiovascular system & hematology, Antibodies, Monoclonal, Humanized, Peritoneal dialysis, Kidney transplantation, 03 medical and health sciences, Systemic lupus erythematosus, 0302 clinical medicine, Renal Dialysis, Prednisone, Internal medicine, medicine, Humans, Lupus Erythematosus, Systemic, Glucocorticoids, Dialysis, business.industry, Lupus nephriti, medicine.disease, Lupus Nephritis, Belimumab, Treatment Outcome, Female, business, Immunosuppressive Agents, medicine.drug
Abstract

Background: Belimumab (Benlysta) is currently approved for the treatment of active Lupus despite standard therapy. Few data are available on the efficacy of this drug in lupus nephritis (LN). Methods: 17 LN female followed in two Nephrology Italian Unit received belimumab for a median period of 36 months (range 6–42 months). The indications were: arthralgia in 3 patients, cutaneous manifestations in 2, residual proteinuria in 8, and the need to reduce steroids for severe side effects in 4. Of interest, 1 patient started therapy during Peritoneal Dialysis and continued after kidney transplantation due to non-responsive arthralgias. Results: Arthralgia and skin manifestations resolved in all patients. Proteinuria normalized in three patients and stabilized in all but one of the others. Steroids were indefinitely stopped in six patients (35%) and reduced to around 40% of the basal dosage in the other patients. During belimumab therapy, three extrarenal and one renal SLE flares were diagnosed accounting for a rate of renal flares of 0.02/patient/year. No major adverse events leading to therapy withdrawal occurred. Clinical case: Arthralgia resolved, immunological parameters improved and prednisone could be reduced within few months in the patient who started belimumab during peritoneal dialysis. After kidney transplantation belimumab was stopped but due to arthralgias unresponsive to standard immunosuppressive therapy it was restarted with success. Conclusions: Belimumab allows the achievement of complete response together with the withdrawal or the reduction of corticosteroids in almost all our patients. Of interest its satisfactory use in a patient in peritoneal dialysis and after kidney transplantation.

Published
2020

5. Novel Therapies in Takayasu Arteritis

Author

Francesca Regola, Martina Uzzo, Paola Toniati, Barbara Trezzi, Renato Alberto Sinico, Franco Franceschini, Regola, F, Uzzo, M, Toniati, P, Trezzi, B, Sinico, R, and Franceschini, F

Subjects
Medicine (General), bDMARD, Takayasu Arteritis, bDMARDs, biologics, heart, novel therapies, General Medicine, Takayasu Arteriti, Review, novel therapie, R5-920, Medicine, biologic
Abstract

Takayasu Arteritis (TAK) is a large-vessel vasculitis that preferentially involves the aorta and its primary branches. Cardiac involvement is frequent in TAK and is a major determinant of the patient's outcome. Glucocorticoids (GC) are the mainstay of therapy for TAK, with high doses of GC effective to induce remission. However, relapses are common and lead to repeated and prolonged GC treatments with high risk of related adverse events. Potential GC toxicity is a major concern, especially because patients with TAK are young and need to be treated for several years, often for the whole life. Conventional immunosuppressive drugs are used in patients with severe manifestations but present some limitations. New therapeutic approaches are needed for patients with refractory disease or contraindications to conventional therapies. Fortunately, major progress has been made in understanding TAK pathogenesis, leading to the development of targeted biotherapies. In particular, IL-6 and TNF-α pathways seems to be the most promising therapeutic targets, with emerging data on Tocilizumab and TNF inhibitors. On the other hand, new insights on JAK-Inhibitors, Rituximab, Ustekinumab and Abatacept have been explored in recent studies. This review summarizes the emerging therapies used in TAK, focusing on the most recent studies on biologics and analyzing their efficacy and safety.

Published
2021

6. Novel Targets for Drug Use in Eosinophilic Granulomatosis With Polyangiitis

Author

Martina Uzzo, Francesca Regola, Barbara Trezzi, Paola Toniati, Franco Franceschini, Renato Alberto Sinico, Uzzo, M, Regola, F, Trezzi, B, Toniati, P, Franceschini, F, and Sinico, R

Subjects
Medicine (General), medicine.medical_specialty, Review, Omalizumab, Therapeutic approach, R5-920, rituximab, novel therapies, Eosinophilic, medicine, Eosinophilic Granulomatosis with Polyangiitis, biologics, heart involvement, Intensive care medicine, Autoimmune disease, business.industry, Eosinophilic Granulomatosis with Polyangiiti, mepolizumab, omalizumab, General Medicine, novel therapie, medicine.disease, Regimen, Medicine, Rituximab, Granulomatosis with polyangiitis, business, biologic, Mepolizumab, medicine.drug
Abstract

Eosinophilic Granulomatosis with Polyangiitis (EGPA) is a rare autoimmune disease characterized by medium and small vessels inflammation. Cardiac vasculitic involvement is one of the most severe manifestations with a significant impact on patients' long-term prognosis: anyway, a specific therapeutic approach for heart involvement in EGPA has not been explored yet. Current regimen consists of a long-term therapy with high dose of glucocorticoids, causing the well-known related-adverse events; immunosuppressive drugs are used in patients with severe manifestations, with some limitations. New therapeutic approaches are needed for patients with refractory disease or contraindications to conventional therapies. The quest for the ideal therapy is going toward a more and more personalized approach: on the one hand, efforts are made to use already existing therapies in the most appropriate way; on the other hand, new insights into EGPA pathogenesis allow the discovery of new targets, as demonstrated by mepolizumab and rituximab, targeting eosinophils, and B-cell compartments. This review summarizes the emerging therapies used in EGPA, focusing on the most recent studies on biologics and analyzing their efficacy and safety.

Published
2021

7. Clinical usefulness of autoantibodies to M-type phospholipase A2 receptor (PLA2R) for monitoring disease activity in idiopathic membranous nephropathy (IMN)

Author

Marco D'Amico, Francesca Pregnolato, Gianpaola Pesce, Umberto Maggiore, Davide Rolla, Francesco Londrino, Giuseppe Ortisi, Antonella Radice, Barbara Trezzi, Federica Ravera, Tiziana Stellato, Renato Alberto Sinico, Pietro Napodano, Domenico Santoro, Radice, A, Trezzi, B, Maggiore, U, Pregnolato, F, Stellato, T, Napodano, P, Rolla, D, Pesce, G, D'Amico, M, Santoro, D, Londrino, F, Ravera, F, Ortisi, G, and Sinico, R

Subjects
Autoantibody, Biomarker, Membranous nephropathy, Phospholipase A2 receptor, Proteinuria, Autoantibodies, Biomarkers, Biopsy, Glomerulonephritis, Membranous, Humans, Receptors, Phospholipase A2, Immunology, Immunology and Allergy, Medicine (all), medicine.medical_specialty, 030232 urology & nephrology, Serum albumin, 030204 cardiovascular system & hematology, Membranous, Gastroenterology, Nephropathy, 03 medical and health sciences, Glomerulonephritis, 0302 clinical medicine, Phospholipase A2, Internal medicine, Receptors, Medicine, biology, business.industry, Antibody titer, Glomerulonephritis, Membranou, medicine.disease, Autoantibodie, biology.protein, Biomarker (medicine), medicine.symptom, Antibody, business, Human
Abstract

Autoantibodies to M-type phospholipase A2 receptor (PLA2R) are specific markers of idiopathic membranous nephropathy (IMN). They can differentiate IMN from other glomerular diseases and primary from secondary forms of MN. Preliminary data suggest that anti-PLA2R antibody titer correlates with disease activity but more solid evidence is needed.To evaluate the performance of anti-PLA2R antibody for monitoring nephropathy activity, 149 anti-PLA2R antibody measurements were performed during the follow-up of 42 biopsy proven IMN consecutive patients. Patients were enrolled either at time of diagnosis (33 cases, inception cohort) or after diagnosis (9 patients, non-inception cohort).Anti-PLA2R detection was performed using the highly sensitive transfected cell-based indirect immunofluorescence (IIFT).Over the follow-up there was a linear time-trend of decreasing proteinuria (P < 0.001), increasing serum albumin (P < 0.001) and decreasing PLA2R antibody levels (P = 0.002). There was a statistically significant association between changes in PLA2R antibody levels and the clinical course of PLA2R-positive IMN. The positive PLA2R serum antibody status was linearly associated with increasing proteinuria and decreasing serum albumin over time, compared with negative antibody status. Moreover, the strong correlation between the clinical conditions and PLA2R antibody levels allowed the prediction of prevalence distribution of patients with active disease, partial and complete remission. Over the course of the follow-up, the probability of halving proteinuria increased 6.5 times after disappearance of PLA2R antibodies.Our data suggest that the serial evaluation of anti-PLA2R antibodies could help in optimal timing and duration of the immunosuppressive therapy, reducing over(under)-treatment and associated side-effects.

Published
2016

8. Glomerular Autoimmune Multicomponents of Human Lupus Nephritis In Vivo (2)

Author

Gabriella Moroni, Corrado Murtas, Piergiorgio Messa, Maricla Galetti, Angela Tincani, Gian Marco Ghiggeri, Giancarlo Barbano, Renato Alberto Sinico, Landino Allegri, Paola Migliorini, Franco Franceschini, Maurizio Bruschi, Alice Bonanni, Pietro Ravani, Giorgio Piaggio, Francesco Scolari, Giovanni Candiano, Federico Pratesi, Alberto Martini, Barbara Trezzi, Antonella Radice, Francesca Brunini, Regina Tardanico, Rita Gatti, Bruschi, M, Galetti, M, Sinico, R, Moroni, G, Bonanni, A, Radice, A, Tincani, A, Pratesi, F, Migliorini, P, Murtas, C, Franceschini, F, Trezzi, B, Brunini, F, Gatti, R, Tardanico, R, Barbano, G, Piaggio, G, Messa, P, Ravani, P, Scolari, F, Candiano, G, Martini, A, Allegri, L, and Ghiggeri, G

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Adolescent, Anti-nuclear antibody, Enolase, SLE, Lupus nephritis, Podocyte, Biology, medicine.disease_cause, Cell Line, Autoimmunity, Histones, Young Adult, chemistry.chemical_compound, Antigen, clinical immunology, immunology and pathology, lupus nephritis, medicine, Humans, Aged, Autoantibodies, Complement C1q, DNA, Female, Lupus Nephritis, Middle Aged, Podocytes, Creatinine, Autoantibody, General Medicine, Lupus Nephriti, medicine.disease, Autoantibodie, Histone, Basic Research, chemistry, Nephrology, Immunology, Nephritis, Human
Abstract

Glomerular planted antigens (histones, DNA, and C1q) are potential targets of autoimmunity in lupus nephritis (LN). However, the characterization of these antigens in human glomeruli in vivo remains inconsistent. We eluted glomerular autoantibodies recognizing planted antigens from laser-microdissected renal biopsy samples of 20 patients with LN. Prevalent antibody isotypes were defined, levels were determined, and glomerular colocalization was investigated. Renal and circulating antibodies were matched, and serum levels were compared in 104 patients with LN, 84 patients with SLE without LN, and 50 patients with rheumatoid arthritis (RA). Autoantibodies against podocyte antigens (anti–α-enolase/antiannexin AI) were also investigated. IgG2 autoantibodies against DNA, histones (H2A, H3, and H4), and C1q were detected in 50%, 55%, and 70% of biopsy samples, respectively. Anti-DNA IgG3 was the unique non-IgG2 anti-DNA deposit, and anti-C1q IgG4 was mainly detected in subepithelial membranous deposits. Anti-H3, anti-DNA, and anti-C1q IgG2 autoantibodies were also prevalent in LN serum, which also contained IgG3 against the antigen panel and anti-C1q IgG4. Serum and glomerular levels of autoantibodies were not strictly associated. High serum levels of all autoantibodies detected, including anti–α-enolase and antiannexin AI, identified LN versus SLE and RA. Anti-H3 and anti–α-enolase IgG2 levels had the most remarkable increase in LN serum and represented a discriminating feature of LN in principal component analysis. The highest levels of these two autoantibodies were also associated with proteinuria>3.5 g/24 hours and creatinine>1.2 mg/dl. Our findings suggest that timely autoantibody characterization might allow outcome prediction and targeted therapies for patients with nephritis.

Published
2015

9. PRIMARY AND SECONDARY GLOMERULONEPHRITIDES 1

Author

Masayuki Iyoda, Taihei Suzuki, Jung Eun Lee, Margherita Conrieri, Angel Sevillano, Katsuyuki Nagatoya, Shankar Prasad Nagaraju, Nicoletta Mezzina, Augusta Praça, A. Malesci, Bjørn Egil Vikse, Tajana Zeljkovic Vrkic, Fumihiko Sasai, Giuseppe Paolo Segoloni, Maki Shinzawa, Terumasa Hayashi, Yutaka Yamaguchi, Maria Elena Donadio, Inês Ferreira, Ioanna Labropoulou, Luca Vergano, Yoshikuni Nagayama, Manuel A Podestà, Guida Meneses, Takayuki Kuragano, Gisele V. Fernandes, Manohar Bairy, Yasuyuki Nagasawa, Ayse Serra Artan, Vedran Premuzic, Barbara Trezzi, Carla Guidi, Manuel Pestana, Makoto Watanabe, Donatella Vizza, Francisco Remédio, Rune Bjørneklett, Niranjan Ambekar, Evangelina Mérida, Narayan Prasad, Ana Cristina Matos, George Toulkeridis, In Mi Han, Enrique Morales, Mohit Kumar Rai, Federica Chiale, Kenichi Sumida, Ann Merethe Vågane, E. Mariz, Adrian Zugravu, Andreas Kronbichler, Michael A. Rudnicki, Praga Manuel, Maria Skoularopoulou, Maria Paola Puccinelli, Mustafa Güllülü, Helena Viana, Loredana Colla, Vasudeva Guddattu, Sung-Bae Park, Sung Jin Moon, Eduardo Gutiérrez, Hirokatsu Atsumi, Junichi Hoshino, Rajeevalochana Parthasarathy, Nimet Aktas, Renzo Bonofilgio, Carla Henriques, Ana Huerta, Jelena Kos, David Cucchiari, Gener Ismail, Renato Alberto Sinico, Anna Varberg Reisæter, Hideki Yamaya, Iuliana Andreiana, Atsushi Yamauchi, Bernardo Faria, Francesca Maria Bosetti, Noriko Hayami, Vincenzo Cantaluppi, Yoshitaka Isaka, Swapnil Karnik, Aydin Turkmen, Alexei Smirnov, Ljiljana Fodor, Jinhyuk Paek, Alberto Boido, Shinichi Uchida, Abdulmecit Yildiz, Takanori Shibata, Sei Sasaki, Xiao-Yan Wei, Ravindra Prabhu, Tiziana Stellato, Roser Torra, Eunah Hwang, Kazuyuki Tasaki, Luigi Biancone, Gutierrez-Solis Elena, Clarissa J. B. Carvalho, Gabriel Mircescu, Ana Teresa Nunes, Elisabet Ars, Tomokazu Okado, Hui Wang, Vanja Ivković, Tushar Anil Dighe, Katsuhito Ihara, Norifumi Hayashi, Roxana Jurubita, Aysegul Oruc, Yasar Caliskan, Mehmet Sukru Sever, Atul Sajgure, Aikaterini Papagianni, Katarzyna Koscielska-Kasprzak, Francesca Leone, Mario Laganović, Archana Buch, Daisuke Komukai, Carina Ferreira, Olga Galkina, Marian Klinger, Sandra Karanović, Manuela Bianciotto, Srinivas Kosuru, Maria Céu Santos, Maurizio Gallieni, Manuel Praga, Yuan-Qing Tian, Ken Iseri, Peter Påhlsson, Kenmei Takaichi, Vikas Agarwal, Manuel Burdese, Aritoshi Kida, Giulio Mengozzi, Giovanni Camussi, Yasutaka Yamamoto, Tomohiro Saito, Seiichi Matsuo, Enyu Imai, Yuki Shindo-Hirai, Edite Pereira, Nida Oztop, Gert Mayer, Tatemitsu Rai, Rosanna Coppo, Hiroshi Okuyama, Dong Ho Shin, Soichiro Iimori, Danilo Lofaro, Hiroki Adachi, Yasemin Ozluk, Maria Alina Gomes de Mattos Cavalcante, Michael C. Carlsson, Bulent Gul, Abhay Sadre, Shunsuke Goto, Vasilii Sipovskii, Kei Fukami, Hiroki Nishiwaki, Tatsuya Suwabe, Daniela Finocchietti, Yuki Matsui, Takshi Nakanishi, Ashwini Sharma, Teresa Papalia, Marijana Cˇorić, Marco D'Amico, Caro-Espada Paula Jara, Francesco Mollica, Licia Peruzzi, Yukihiro Wada, Roberta Camilla, Agata Mollica, E. O. Bogdanova, Raluca Bobeica, Cai-Li Wang, Eugen Mandache, Francesco Reggiani, Joaquim Calado, Li Lv, Elena Saganova, Fernanda Carvalho, Halil Yazici, Yan-Hui Zhang, Elisa Loiacono, Christos Bantis, Teresa Cavero, Salvatore Badalamenti, Hakon Leffler, Sigrid Lundberg, Tarun Jeloka, Ligia Petrescu, Luca Besso, Alline S. A. Oliveira, Stratis Kasimatis, Thomas Knoop, Davide Medica, Germana Daidola, E. Hernandez, Mana Yahiro, Rojas-Rivera Jorge Enrique, João M. Frazão, Kouki Mise, Toshiaki Suzuki, Yoshihiro Kuno, Atul Mulay, Jun Ito, Katarzyna Gniewek, George Efstratiadis, Marijana Ćorić, Jara Caro, Maria Stangou, Aysun Aksoy, Fernando Nolasco, Katarzyna Jakuszko, Paolo Gigliotti, Tae Hyun Yoo, Takeshi Hasegawa, Hideki Fujii, Ricardo Neto, Simona Stancu, Susana Sampaio, Camila Barbosa L Oliveira, Sindhura Lakshmi Koulmane Laxminarayana, Alaattin Yildiz, Shigeo Hara, Kei Matsumoto, Ludmila Taran, Nikoleta Maria Kouri, Shinichi Nishi, Andreea Avram, Zivka Dika, Nobuharu Kaneshima, Charan Bhadrappa Bale, Gian Marco Ghiggeri, Ashio Yoshimura, Lei Nan, Rachele Gallo, Keiji Fujimoto, Alessandro Amore, Mårten Segelmark, Luís H. B. C. Sette, Francesca Brunini, Bojan Jelaković, Lucila Maria Valente, Ryohei Yamamoto, Andreea Andronesi, Julia Kerschbaum, Inna Lastauka, Mohamed R. Daha, Akhilesh Jaiswal, Ni-Ya Jia, Jayraj Korpe, Shinichi Akiyama, Domenico Santoro, Marc A. Seelen, Ebru Acikgoz, Shoichi Maruyama, Anna Perri, Hitoshi Yokoyama, Magdalena Krajewska, Brijesh Yadav, Hyungjong Kim, Irina Zubina, Tatsuya Shoji, Yoshifumi Ubara, Claudio Angelini, Margareta Fištrek Prlić, Ian Proletov, Kentaro Nakai, Isin Kilicaslan, Antonella Radice, Prachi Kate, Sayuri Hamahata, Jose Antonio Moreno, and Marijana Zivko

Subjects
Transplantation, medicine.medical_specialty, Pediatrics, Primary (chemistry), Nephrology, business.industry, Alternative medicine, medicine, business, Intensive care medicine
Published
2014

10. Glomerular autoimmune multicomponents of human lupus nephritis in vivo: α-enolase and annexin AI

Author

Piergiorgio Messa, Maricla Galetti, Maurizio Bruschi, Paola Migliorini, Laura Bianchi, Renato Alberto Sinico, Angela Tincani, Giancarlo Barbano, Andrea Scaloni, Chiara D'Ambrosio, Alice Bonanni, Landino Allegri, Federico Pratesi, Maria Luisa Carnevali, Giovanni Candiano, Gian Marco Ghiggeri, Regina Tardanico, Pietro Ravani, Alberto Martini, Michael P. Madaio, Gabriella Moroni, Francesco Scolari, Agata Giallongo, Franco Franceschini, Barbara Trezzi, Antonella Radice, Rita Gatti, Beatrice Bianco, Corrado Murtas, Bruschi, M, Sinico, R, Moroni, G, Pratesi, F, Migliorini, P, Galetti, M, Murtas, C, Tincani, A, Madaio, M, Radice, A, Franceschini, F, Trezzi, B, Bianchi, L, Giallongo, A, Gatti, R, Tardanico, R, Scaloni, A, D'Ambrosio, C, Carnevali, M, Messa, P, Ravani, P, Barbano, G, Bianco, B, Bonanni, A, Scolari, F, Martini, A, Candiano, G, Allegri, L, and Ghiggeri, G

Subjects
Male, Proteomics, Pathology, Mice, Inbred MRL lpr, Biopsy, Kidney Glomerulus, Lupus nephritis, Mice, SCID, lupus nephriti, medicine.disease_cause, Autoimmunity, Mice, Inbred BALB C, Annexin A1, Mice, Inbred BALB C, Tumor, medicine.diagnostic_test, General Medicine, Middle Aged, Autoantibodie, Lupus Nephritis, DNA-Binding Proteins, Nephrology, GN, Monoclonal, Immunohistochemistry, Female, Human, immunology and pathology, lupus nephritis, Adolescent, Adult, Animals, Autoantibodies, Biomarkers, Tumor, Humans, Immunoglobulin G, Phosphopyruvate Hydratase, Tumor Suppressor Proteins, Young Adult, medicine.medical_specialty, DNA-Binding Protein, Enolase, Biology, SCID, Inbred MRL lpr, medicine, Tumor Suppressor Protein, Animal, Autoantibody, Proteomic, medicine.disease, Basic Research, Immunology, Kidney Glomerulu, Biomarkers
Abstract

Renal targets of autoimmunity in human lupus nephritis (LN) are unknown. We sought to identify autoantibodies and glomerular target antigens in renal biopsy samples from patients with LN and determine whether the same autoantibodies can be detected in circulation. Glomeruli were microdissected from biopsy samples of 20 patients with LN and characterized by proteomic techniques. Serum samples from large cohorts of patients with systemic lupus erythematosus (SLE) with and without LN and other glomerulonephritides were tested. Glomerular IgGs recognized 11 podocyte antigens, with reactivity varying by LN pathology. Notably, IgG2 autoantibodies against α-enolase and annexin AI were detected in 11 and 10 of the biopsy samples, respectively, and predominated over other autoantibodies. Immunohistochemistry revealed colocalization of α-enolase or annexin AI with IgG2 in glomeruli. High levels of serum anti–α-enolase (>15 mg/L) IgG2 and/or anti-annexin AI (>2.7 mg/L) IgG2 were detected in most patients with LN but not patients with other glomerulonephritides, and they identified two cohorts: patients with high anti–α-enolase/low anti-annexin AI IgG2 and patients with low anti–α-enolase/high anti-annexin AI IgG2. Serum levels of both autoantibodies decreased significantly after 12 months of therapy for LN. Anti–α-enolase IgG2 recognized specific epitopes of α-enolase and did not cross-react with dsDNA. Furthermore, nephritogenic monoclonal IgG2 (clone H147) derived from lupus-prone MRL-lpr/lpr mice recognized human α-enolase, suggesting homology between animal models and human LN. These data show a multiantibody composition in LN, where IgG2 autoantibodies against α-enolase and annexin AI predominate in the glomerulus and can be detected in serum.

Published
2014

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