Litcius/Paper detail

Halting targeted and collateral damage to red blood cells by the complement system

Marit Jalink, Esther C. W. de Boer, Dorothea Evers, M. Q. Havinga, Josephine M. I. Vos, Sacha Zeerleder, Masja de Haas, Ilse Jongerius

2021Seminars in Immunopathology19 citationsDOIOpen Access PDF

Abstract

The complement system is an important defense mechanism against pathogens; however, in certain pathologies, the system also attacks human cells, such as red blood cells (RBCs). In paroxysmal nocturnal hemoglobinuria (PNH), RBCs lack certain complement regulators which sensitize them to complement-mediated lysis, while in autoimmune hemolytic anemia (AIHA), antibodies against RBCs may initiate complement-mediated hemolysis. In recent years, complement inhibition has improved treatment prospects for these patients, with eculizumab now the standard of care for PNH patients. Current complement inhibitors are however not sufficient for all patients, and they come with high costs, patient burden, and increased infection risk. This review gives an overview of the underlying pathophysiology of complement-mediated hemolysis in PNH and AIHA, the role of therapeutic complement inhibition nowadays, and the high number of complement inhibitors currently under investigation, as for almost every complement protein, an inhibitor is being developed. The focus lies with novel therapeutics that inhibit complement activity specifically in the pathway that causes pathology or those that reduce costs or patient burden through novel administration routes.

Topics & Concepts

Paroxysmal nocturnal hemoglobinuriaEculizumabComplement systemHemolysisImmunologyCD59Complement (music)Complement membrane attack complexMedicineAlternative complement pathwayAntibodyComplement component 5CytolysisBiologyCytotoxicityIn vitroPhenotypeComplementationBiochemistryGeneComplement system in diseasesBlood groups and transfusionErythrocyte Function and Pathophysiology