Pre-diagnostic blood immune markers, incidence and progression of B-cell lymphoma and multiple myeloma: Univariate and functionally informed multivariate analyses.

Roel Vermeulen,Salvatore Panico,Panagiotis Georgiadis,Raphaële Castagné,Ioannis Valavanis,Barbara Bodinier,Chuhsing Kate Hsiao,Benoît Liquet,Soterios A Kyrtopoulos,Riikka Airaksinen,Fatemeh Saberi Hosnijeh,Thomas Lundh,Lützen Portengen,Rosario Tumino,Domenico Palli,Marco De Santis,Manolis Kogevinas,Maria Botsivali,Hung Hung,Vittorio Krogh,Euripides G Stephanou,Aristotelis Chatziioannou,Hector C Keun,Per Lenner,Antonis Myridakis,Benedetta Bendinelli,Lucia Fazzo,Beatrice Melin,Thomas Fleming,Panu Rantakokko,Toby J Athersuch,Sarah Fleming,Pietro Comba,Carlotta Sacerdote,Ingvar A Bergdahl,Marc Chadeau‐Hyam,Hannu Kiviranta,Kuo Liong Chien ,Ann Sofie Johansson ,Rachel S Kelly ,Henk M Lokhorst ,Wen‐Chung Lee ,Jos Kleinjans ,Wei-Jen Chen ,Göran Hallmans ,Javiera Garrido-Manriquez ,Po-Chen Kuo ,Mark S Gilthorpe ,Päivi Ruokojärvi ,Yu Kang Tu ,Theo M C M De Kok ,Paolo Víneis ,Shu-Fen Liao

doi:10.1002/ijc.31536

Abstract

Recent prospective studies have shown that dysregulation of the immune system may precede the development of B‐cell lymphomas (BCL) in immunocompetent individuals. However, to date, the studies were restricted to a few immune markers, which were considered separately. Using a nested case–control study within two European prospective cohorts, we measured plasma levels of 28 immune markers in samples collected a median of 6 years before diagnosis (range 2.01–15.97) in 268 incident cases of BCL (including multiple myeloma [MM]) and matched controls. Linear mixed models and partial least square analyses were used to analyze the association between levels of immune marker and the incidence of BCL and its main histological subtypes and to investigate potential biomarkers predictive of the time to diagnosis. Linear mixed model analyses identified associations linking lower levels of fibroblast growth factor‐2 (FGF‐2 p = 7.2 × 10−4) and transforming growth factor alpha (TGF‐α, p = 6.5 × 10−5) and BCL incidence. Analyses stratified by histological subtypes identified inverse associations for MM subtype including FGF‐2 (p = 7.8 × 10−7), TGF‐α (p = 4.08 × 10−5), fractalkine (p = 1.12 × 10−3), monocyte chemotactic protein‐3 (p = 1.36 × 10−4), macrophage inflammatory protein 1‐alpha (p = 4.6 × 10−4) and vascular endothelial growth factor (p = 4.23 × 10−5). Our results also provided marginal support for already reported associations between chemokines and diffuse large BCL (DLBCL) and cytokines and chronic lymphocytic leukemia (CLL). Case‐only analyses showed that Granulocyte‐macrophage colony stimulating factor levels were consistently higher closer to diagnosis, which provides further evidence of its role in tumor progression. In conclusion, our study suggests a role of growth‐factors in the incidence of MM and of chemokine and cytokine regulation in DLBCL and CLL.

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