Abbonarsi

Dissecting the mechanism of action of intravenous immunoglobulin in human autoimmune disease: Lessons from therapeutic modalities targeting Fc? receptors - 05/09/20

Doi : 10.1016/j.jaci.2020.06.036 
Anthony Shock, PhD a, David Humphreys, PhD a, Falk Nimmerjahn, PhD b, c,
a UCB Pharma, Slough, United Kingdom 
b Institute of Genetics, Department of Biology, Friedrich Alexander University of Erlangen-Nuremberg, Erlangen, Germany 
c Medical Immunology Campus Erlangen, Erlangen, Germany 

Corresponding author: Falk Nimmerjahn, PhD, Institute of Genetics, Department of Biology, Friedrich Alexander University of Erlangen-Nuremberg, Erwin-Rommelstr. 3, 91054 Erlangen, Germany.Institute of GeneticsDepartment of BiologyFriedrich Alexander University of Erlangen-NurembergErwin-Rommelstr. 3Erlangen91054Germany

Abstract

Since the first description of the administration of high doses of pooled serum IgG, also referred to as intravenous IgG (IVIg) therapy, as being able to ameliorate various autoimmune diseases, researchers have been investigating which molecular and cellular pathways underlie IVIg activity. Apart from trying to understand the obvious conundrum that IgG can trigger both autoimmune pathology and resolution of inflammation, the rapidly expanding use of IVIg has led to a lack of availability of this primary blood product, providing a strong rationale for developing recombinant alternatives. During the last decade, a tremendous number of novel insights into IVIg activity brought the goal of replacing IVIg within reach, at least in select indications, and has led to the initiation of several clinical trials. At the forefront of this effort is the modulation of autoantibody half-life and blocking access of autoantibodies to fragment cystallizable γ receptors (Fcγ receptors). In this rostrum article, we will briefly discuss current models of IVIg activity, followed by a more specific focus on novel therapeutic avenues that are entering the clinic and may replace IVIg in the future.

Il testo completo di questo articolo è disponibile in PDF.

Key words : Intravenous immunoglobulin, Fcγ receptors, autoimmunity, inflammation, neonatal Fc receptor

Abbreviations used : CIA, CIDP, Fc, FcγR, FcRn, IC, ITP, IVIg, SLE


Mappa


 This article was written by the authors with editorial support funded by UCB Pharma in accordance with Good Publications Practice (GPP3) guidelines (gpp3). The article was reviewed and approved for publication by all authors and the sponsor. The authors acknowledge Linda Feighery, PhD, CMPP, and Veronica Porkess, PhD, CMPP, of UCB Pharma for publication and editorial support.
 Disclosure of potential conflict of interest: A. Shock and D. Humphreys are employees of UCB Pharma and hold stock and/or stock options. UCB Pharma is the manufacturer and sponsor of rozanolixizumab, a neonatal fragment crystallizable (Fc) receptor (FcRn) inhibitor, which is currently being investigated in clinical trials in a number of autoimmune disorders. F. Nimmerjahn has received personal fees from UCB Pharma for consultancy (advisory board) conducted outside of the submitted work.


© 2020  The Authors. Pubblicato da Elsevier Masson SAS. Tutti i diritti riservati.
Aggiungere alla mia biblioteca Togliere dalla mia biblioteca Stampare
Esportazione

    Citazioni Export

  • File

  • Contenuto

Vol 146 - N° 3

P. 492-500 - Settembre 2020 Ritorno al numero
Articolo precedente Articolo precedente
  • Targeting FcRn for immunomodulation: Benefits, risks, and practical considerations
  • Hans-Hartmut Peter, Hans D. Ochs, Charlotte Cunningham-Rundles, Donald C. Vinh, Peter Kiessling, Bernhard Greve, Stephen Jolles
| Articolo seguente Articolo seguente
  • The Editors’ Choice
  • Zuhair K. Ballas, Associate Editors of the JACI

Benvenuto su EM|consulte, il riferimento dei professionisti della salute.
L'accesso al testo integrale di questo articolo richiede un abbonamento.

Già abbonato a @@106933@@ rivista ?

Il mio account


Dichiarazione CNIL

EM-CONSULTE.COM è registrato presso la CNIL, dichiarazione n. 1286925.

Ai sensi della legge n. 78-17 del 6 gennaio 1978 sull'informatica, sui file e sulle libertà, Lei puo' esercitare i diritti di opposizione (art.26 della legge), di accesso (art.34 a 38 Legge), e di rettifica (art.36 della legge) per i dati che La riguardano. Lei puo' cosi chiedere che siano rettificati, compeltati, chiariti, aggiornati o cancellati i suoi dati personali inesati, incompleti, equivoci, obsoleti o la cui raccolta o di uso o di conservazione sono vietati.
Le informazioni relative ai visitatori del nostro sito, compresa la loro identità, sono confidenziali.
Il responsabile del sito si impegna sull'onore a rispettare le condizioni legali di confidenzialità applicabili in Francia e a non divulgare tali informazioni a terzi.


Tutto il contenuto di questo sito: Copyright © 2024 Elsevier, i suoi licenziatari e contributori. Tutti i diritti sono riservati. Inclusi diritti per estrazione di testo e di dati, addestramento dell’intelligenza artificiale, e tecnologie simili. Per tutto il contenuto ‘open access’ sono applicati i termini della licenza Creative Commons.