Comparison of Monoclonal Gammopathies Linked to Poliovirus or Coxsackievirus vs. Other Infectious Pathogens

Author:

Harb Jean,Mennesson Nicolas,Lepetit Cassandra,Fourny Maeva,Louvois Margaux,Bosseboeuf Adrien,Allain-Maillet Sophie,Decaux Olivier,Moreau Caroline,Tallet Anne,Piver EricORCID,Moreau Philippe,Salle Valéry,Bigot-Corbel EdithORCID,Hermouet SylvieORCID

Abstract

Chronic stimulation by infectious pathogens or self-antigen glucosylsphingosine (GlcSph) can lead to monoclonal gammopathy of undetermined significance (MGUS) and multiple myeloma (MM). Novel assays such as the multiplex infectious antigen microarray (MIAA) and GlcSph assays, permit identification of targets for >60% purified monoclonal immunoglobulins (Igs). Searching for additional targets, we selected 28 purified monoclonal Igs whose antigen was not represented on the MIAA and GlcSph assays; their specificity of recognition was then analyzed using microarrays consisting of 3760 B-cell epitopes from 196 pathogens. The peptide sequences PALTAVETG and PALTAAETG of the VP1 coat proteins of human poliovirus 1/3 and coxsackievirus B1/B3, respectively, were specifically recognized by 6/28 monoclonal Igs. Re-analysis of patient cohorts showed that purified monoclonal Igs from 10/155 MGUS/SM (6.5%) and 3/147 MM (2.0%) bound to the PALTAVETG or PALTAAETG epitopes. Altogether, PALTAV/AETG-initiated MGUS are not rare and few seem to evolve toward myeloma.

Funder

Janssen Pharmaceuticals

Ligue Contre le Cancer

Canceropole Grand Ouest

Region Pays de la Loire

Publisher

MDPI AG

Subject

General Medicine

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