Blockade of Alternative Complement Pathway in Dense Deposit Disease

AuroreBerthe-Aucejo; MathieuSacquépée; MarcFila; MichelPeuchmaur; EmiliaPerrier-Cornet; VéroniqueFrémeaux-Bacchi; GeorgesDeschênes

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Blockade of Alternative Complement Pathway in Dense Deposit Disease

机译：致密矿床疾病的替代补体途径的封锁

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A patient aged 17 with dense deposit disease associated with complement activation, circulating C3 Nef, and Factor H mutation presented with nephrotic syndrome and hypertension. Steroid therapy, plasma exchange, and rituximab failed to improve proteinuria and hypertension despite a normalization of the circulating sC5b9 complex. Eculizumab, a monoclonal antibody directed against C5, was used to block the terminal product of the complement cascade. The dose was adapted to achieve a CH50 below 10%, but proteinuria and blood pressure were not improved after 3 months of treatment.

机译：一名17岁的患者，患有致密性沉积病，伴有补体激活，循环C3 Nef和H因子突变，并伴有肾病综合征和高血压。尽管循环中的sC5b9复合物正常化，但类固醇疗法，血浆置换和利妥昔单抗未能改善蛋白尿和高血压。 Eculizumab是一种针对C5的单克隆抗体，用于阻断补体级联反应的终产物。调整剂量可使CH50低于10％，但治疗3个月后蛋白尿和血压并未改善。

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《Case Reports in Nephrology》 |2014年第1期|共4页
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AuroreBerthe-Aucejo; MathieuSacquépée; MarcFila; MichelPeuchmaur; EmiliaPerrier-Cornet; VéroniqueFrémeaux-Bacchi; GeorgesDeschênes;
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1. Glomeruli of Dense Deposit Disease contain components of the alternative and terminal complement pathway [J] . Sanjeev Sethi, Jeffrey D Gamez, Julie A Vrana, Kidney international. . 2009,第9期

机译：致密病的肾小球包含替代途径和终末补体途径的成分
2. Alternative pathway dysfunction in kidney disease: A case report and review of dense deposit disease and C3 Glomerulopathy [J] . HawfieldA., IskandarS.S., SmithR.J.H. American Journal of Kidney Diseases: The official journal of the National Kidney Foundation . 2013,第5期

机译：肾脏疾病的替代途径功能障碍：一例病例报告和致密性沉积物疾病和C3肾小球病回顾
3. Causes of alternative pathway dysregulation in dense deposit disease [J] . ZhangY., MeyerN.C., WangK., Clinical journal of the American Society of Nephrology: CJASN . 2012,第2期

机译：致密矿床病中替代途径失调的原因
4. Humanized Recombinant Vaccinia Virus Complement Control Protein (hrVCP) with Three Amino Acid Changes, H98Y, E102K, and E120K Creating an Additional Putative Heparin Binding Site, Is 100-fold More Active Than rVCP in Blocking Both Classical and Alternative Complement Pathways [C] . YOHANNES T. GHEBREMARIAM, ODUTAYO O. ODUNUGA, KRISTEN JANSE, International Conference on Natural Products and Molecular Medicine . 2005

机译：人源化重组疫苗病毒补蛋白（HRVCP）具有三个氨基酸变化，H98Y，E102K和E120K产生另外的肝素结合位点，比RVCP在阻断经典和替代的补体途径时，100倍。
5. The role of the alternative pathway of the complement system in the development of dense deposit disease. [D] . Abeleda, Maria Asuncion Abrera. 2010

机译：补体系统替代途径在致密性沉积物疾病发展中的作用。
6. Blockade of Alternative Complement Pathway in Dense Deposit Disease [O] . Aurore Berthe-Aucejo, Mathieu Sacquépée, Marc Fila, 2014

机译：致密矿床疾病的替代补体途径的封锁
7. Glomeruli of Dense Deposit Disease contain components of the alternative and terminal complement pathway [O] . Sethi Sanjeev, Gamez Jeffrey D., Vrana Julie A., 2009

机译：致密病的肾小球包含替代途径和终末补体途径的成分

Blockade of Alternative Complement Pathway in Dense Deposit Disease

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