How I treat paroxysmal nocturnal hemoglobinuria

Slides:

Advertisements

Similar presentations

Developing Immunotherapy for Autoimmune Diseases

Advertisements

Paroxysmal Nocturnal Hemoglobinuria Paul M. Johnson Department of Internal Medicine University of North Carolina Hospitals April 6, 2010.

Complement regulator and disease MEMBERS: 刘婷婷孙满意李晓露宗广鑫张桂李刚.

MLAB 1415: H EMATOLOGY K ERI B ROPHY -M ARTINEZ Hemolytic Anemias: Membrane Defects Part Two.

THE COMPLEMENT SYSTEM. The complement system The complement system is a set of plasma proteins that act in a cascade to attack and kill extracellular.

Proteins of Immunology

The Complement System A group of > 30 plasma proteins which comprise the primary soluble component of innate immunity. Rapidly activated in response to.

Antigenic Surface C1r and C1s Enzymes Associate with C1q to form C1 CH 2 Conformational Change C1r 2 - C1s 2 C1q Ca 2+ Fig. 9.1 C1 activation by an antibody.

The Complement system. objectives Factors involved in the immune response The complement system General properties of complement Cascade activation complement.

Date of download: 6/26/2016 Copyright © 2016 American Medical Association. All rights reserved. From: Complement, Age-Related Macular Degeneration and.

Paroxysmal Nocturnal Hemoglobinuria

Summary. The main function of the immune system Defense Autotolerance Immune supervision Antigens Exoantigeny (allergens, superantigeny...) autoantigens.

Eculizumab (Approved investigational drug) DB01257

IMMUNE HEMOLYSIS Definition : red cell life span is shortened because abnormalities in the components of the immune system are specifically directed against.

Regulation of monocyte procoagulant activity in acute myocardial infarction: role of tissue factor and tissue factor pathway inhibitor-1 by Ilka Ott, Martin.

Complement Ali Al Khader, MD Faculty of Medicine

Moss-made Biopharmaceuticals

Oligoclonal expansion of T lymphocytes with multiple second-site mutations leads to Omenn syndrome in a patient with RAG1-deficient severe combined immunodeficiency.

Strategy for the treatment of acute myelogenous leukemia based on folate receptor β–targeted liposomal doxorubicin combined with receptor induction using.

Experimental Hematology

CD146 (Mel-CAM), an adhesion marker of endothelial cells, is a novel marker of lymphocyte subset activation in normal peripheral blood by Mohamed F. Elshal,

وظایف کمپلمان اپسونیزاسیون به منظور افزایش فاگوسیتوز

Eculizumab salvage therapy for delayed hemolysis transfusion reaction in sickle cell disease patients by Guillaume Dumas, Anoosha Habibi, Thierry Onimus,

Figure 1 Pathways of complement activation

Figure 2 Overview of the complement system

Complement functions اپسونیزاسیون و فاگوسیتوز تحریک پاسخ های التهابی

The spectrum of PIG-A gene mutations in aplastic anemia/paroxysmal nocturnal hemoglobinuria (AA/PNH): a high incidence of multiple mutations and evidence.

وظایف سیستم کمپلمان اپسو.نیزاسیون برای افزایش فاگوسیتوز

CD6 Ligation Modulates the Bcl-2/Bax Ratio and Protects Chronic Lymphocytic Leukemia B Cells From Apoptosis Induced by Anti-IgM by Lyda M. Osorio, Angelina.

Clinical efficacy and management of monoclonal antibodies targeting CD38 and SLAMF7 in multiple myeloma by Niels W. C. J. van de Donk, Philippe Moreau,

by Wolfram Springer, Alexander von Ruecker, and Roswitha Dickerhoff

Sustained signaling through the B-cell receptor induces Mcl-1 and promotes survival of chronic lymphocytic leukemia B cells by Aleksandar Petlickovski,

Elements of the Immune System: Complement

by Alexander Röth, Andreas Hüttmann, Russell P

Sanjeev Sethi, Carla M. Nester, Richard J.H. Smith

Essential role of the C5a receptor in E coli–induced oxidative burst and phagocytosis revealed by a novel lepirudin-based human whole blood model of inflammation.

Detection of Trisomy 12 and Rb-Deletion in CD34+ Cells of Patients With B-Cell Chronic Lymphocytic Leukemia by B. Gahn, C. Schäfer, J. Neef, C. Troff,

by Anne-lie Ståhl, Lisa Sartz, and Diana Karpman

FcRL6, a new ITIM-bearing receptor on cytolytic cells, is broadly expressed by lymphocytes following HIV-1 infection by Timothy J. Wilson, Rachel M. Presti,

The clonal selection model of immunogenesis

A Strong Expression of CD44-6v Correlates With Shorter Survival of Patients With Acute Myeloid Leukemia by S. Legras, U. Günthert, R. Stauder, F. Curt,

Highly homologous T-cell receptor beta sequences support a common target for autoreactive T cells in most patients with paroxysmal nocturnal hemoglobinuria.

by Anita Hill, Peter Hillmen, Stephen J

Activated monocytes in sickle cell disease: potential role in the activation of vascular endothelium and vaso-occlusion by John D. Belcher, Paul H. Marker,

Cytokine-Release Syndrome in Patients With B-Cell Chronic Lymphocytic Leukemia and High Lymphocyte Counts After Treatment With an Anti-CD20 Monoclonal.

Figure 3 Therapeutic intervention in the complement cascade

Figure 4 Cascade system activation on a biomaterial surface

Innate Immune Responses to Transplants

Griet A. Van Roey, PhD, Christopher C

A fully recombinant human IgG1 Fc multimer (GL-2045) inhibits complement-mediated cytotoxicity and induces iC3b by Hua Zhou, Henrik Olsen, Edward So, Emmanuel.

Complement Ali Al Khader, MD Faculty of Medicine

by Katalin Kis-Toth, Gaurav Manohar Rajani, Allison Simpson, Kate L

Terry Kotrla, MS, MT(ASCP)BB

Figure 1 The complement system and its targets

Complement Complement proteins become activated when they encounter antigen Cascading enzyme reactions concentrate activated complement at infection site.

T exosomes bind MAdCAM-1 via RA-increased integrin α4β7.

Fleeting Activation of Ionotropic Glutamate Receptors Sensitizes Cortical Neurons to Complement Attack Zhi-Qi Xiong, James O McNamara Neuron Volume.

Overview The complement system is part of the innate immune system (vs adaptive) It is named “complement system” because it was first identified as a heat-labile.

Lec.8 COMPLEMENT SYSTEM.

SUCROSE HEMOLYSIS TEST

Complement disorders and hereditary angioedema

Novel aspects of complement in kidney injury

Targeting CD47 in Sézary syndrome with SIRPαFc

Eculizumab Therapy in Children with Severe Hematopoietic Stem Cell Transplantation– Associated Thrombotic Microangiopathy Sonata Jodele, Tsuyoshi Fukuda,

Bacterial killing by complement requires membrane attack complex formation via surface‐bound C5 convertases ASchematic overview of complement activation.

HUS and atypical HUS by T. Sakari Jokiranta Blood

The complement system in the airway epithelium: An overlooked host defense mechanism and therapeutic target? Hrishikesh S. Kulkarni, MD, MSCI, M. Kathryn.

Consequences of complement activation.

Flt-1, vascular endothelial growth factor receptor 1, is a novel cell surface marker for the lineage of monocyte-macrophages in humans by Asako Sawano,

Presentation transcript:

How I treat paroxysmal nocturnal hemoglobinuria by Robert A. Brodsky Blood Volume 113(26):6522-6527 June 25, 2009 ©2009 by American Society of Hematology

Multiparameter flow cytometry analysis of peripheral blood in PNH Multiparameter flow cytometry analysis of peripheral blood in PNH. (A-D) Aplastic anemia patient with small (2%) PNH clone; (E-H) classic PNH patient. Multiparameter flow cytometry analysis of peripheral blood in PNH. (A-D) Aplastic anemia patient with small (2%) PNH clone; (E-H) classic PNH patient. (A,E) Forward scatter (FSC)/side scatter (SSC) display showing initial gate to exclude lymphocytes and debris. (B,F) Granulocytes (green) are identified as bright CD15 and low CD33, whereas monocytes (blue) are bright CD33 and low CD15. (C,G) Population of GPI anchor protein–deficient granulocytes showing lack of staining with both anti-CD24 and FLAER. (D,H) Population of GPI anchor protein–deficient monocytes showing lack of staining with both anti-CD14 and FLAER. Robert A. Brodsky Blood 2009;113:6522-6527 ©2009 by American Society of Hematology

Structure of eculizumab. Structure of eculizumab. Eculizumab was engineered to reduce immunogenicity and eliminate effector function. Human IgG2 and IgG4 heavy-chain sequences were combined to form a hybrid constant region that is unable to bind Fc receptors or to activate the complement cascade. Eculizumab exhibits high affinity for human C5, effectively blocking its cleavage and downstream proinflammatory and cell lytic properties. Reprinted from Rother et al36 with permission. Robert A. Brodsky Blood 2009;113:6522-6527 ©2009 by American Society of Hematology

Overview of the complement cascade. Overview of the complement cascade. Classic, alternative, and lectin pathways converge at the point of C3 activation. The lytic pathway is initiated with the formation of C5 convertase and leads to the assembly of the C5, C6, C7, C8, (n) C9 membrane attack complex. Eculizumab is a monoclonal antibody that binds to C5, thereby preventing the formation of C5a and C5b. C5b is the initiating component of the MAC. Reprinted from Brodsky37 with permission. Robert A. Brodsky Blood 2009;113:6522-6527 ©2009 by American Society of Hematology

Reduction in intravascular hemolysis during treatment with eculizumab. Reduction in intravascular hemolysis during treatment with eculizumab. Mean levels of lactate dehydrogenase reflect the degree of hemolysis from baseline to week 52. The dashed line represents the upper limit of the normal range for lactate dehydrogenase (normal range, 103-223 U/L). In eculizumab-treated patients, the mean level of lactate dehydrogenase was rapidly reduced to just above the upper limit of the normal range. In the placebo group, the mean level of lactate dehydrogenase remained highly elevated. The arrow represents the transition of placebo-treated patients to eculizumab treatment in the phase 3 extension study, at which time levels of lactate dehydrogenase rapidly reduced to near normal values. Reprinted from Rother et al36 with permission. Robert A. Brodsky Blood 2009;113:6522-6527 ©2009 by American Society of Hematology