American Association for Cancer Research
Browse
- No file added yet -

Figure S1 from ABO Blood Group IgM Isoagglutinins Interact with Tumor-Associated O-Glycan Structures in Pancreatic Cancer

Download (220.89 kB)
figure
posted on 2023-03-31, 18:16 authored by Bianca T. Hofmann, Anne Stehr, Thorsten Dohrmann, Cenap Güngör, Lena Herich, Jens Hiller, Sönke Harder, Florian Ewald, Florian Gebauer, Michael Tachezy, Clarissa Precht, Jakob R. Izbicki, Maximilian Bockhorn, Christoph Wagener, Gerrit Wolters-Eisfeld

Supplemental Figure S1: Relative Survival of PDAC patients with different blood groups. Kaplan Meier survival plot shows relative survival of PDAC patients in blood group O (blue), blood group A (green), blood group B (yellow) and blood group AB (purple). No significant statistical association was observed.

History

ARTICLE ABSTRACT

Purpose: The ABO gene locus is associated with the risk of developing pancreatic ductal adenocarcinoma (PDAC) resulting in an increased incidence in individuals with non-O blood groups. Up to 90% of PDAC specimens display alterations in mucin type O-GalNAc glycosylation. Because aberrant O-GalNAc glycans (Tn and T antigen) are structurally related to blood group A and B glycans, we investigated the role of IgM isoagglutinins in PDAC.Experimental Design: Binding studies of IgM isoagglutinins toward blood group A, B, Tn antigen, and T antigen glycoconjugates from patients with PDAC and healthy individuals were conducted. Isoagglutinin titers and total IgM were compared between patients with PDAC and control group. An anti-A antibody was used for immunoprecipitation of aberrant O-glycosylated tumor proteins and subsequent mass spectromic analysis.Results: We found that IgM isoagglutinins bind blood group antigens, Tn and T glycoconjugates as well as tumor-derived glycoproteins. Blood group A isoagglutinins exhibited a strong binding toward blood group B antigen and T antigen, whereas blood group B showed binding to blood group A antigen and Tn antigen. Furthermore, we confirmed a decreased frequency in individuals with blood group O and observed a significant decrease of IgM isoagglutinin titers in PDAC sera compared with control sera, whereas total IgM levels were unaltered. We identified new PDAC-derived O-GalNAc glycoproteins by mass spectrometry using a blood group A-specific antibody.Conclusion: Our data elucidated a novel interaction of blood group IgM isoagglutinins and PDAC O-GalNAc glycoproteins that may contribute to the pathogenesis and progression of pancreatic cancer. Clin Cancer Res; 20(23); 6117–26. ©2014 AACR.