Distinct immune characteristics distinguish hereditary and idiopathic chronic pancreatitis
Bomi Lee, Julia Z. Adamska, Hong Namkoong, Melena D. Bellin, Josh Wilhelm, Gregory L. Szot, David M. Louis, Mark M. Davis, Stephen J. Pandol, Aida Habtezion
Bomi Lee, Julia Z. Adamska, Hong Namkoong, Melena D. Bellin, Josh Wilhelm, Gregory L. Szot, David M. Louis, Mark M. Davis, Stephen J. Pandol, Aida Habtezion
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Concise Communication Gastroenterology Immunology

Distinct immune characteristics distinguish hereditary and idiopathic chronic pancreatitis

Abstract

Chronic pancreatitis (CP) is considered an irreversible fibroinflammatory pancreatic disease. Despite numerous animal model studies, questions remain about local immune characteristics in human CP. We profiled pancreatic immune cell characteristics in control organ donors and CP patients including those with hereditary and idiopathic CP undergoing total pancreatectomy with islet autotransplantation. Flow cytometric analysis revealed a significant increase in the frequency of CD68+ macrophages in idiopathic CP. In contrast, hereditary CP samples showed a significant increase in CD3+ T cell frequency, which prompted us to investigate the T cell receptor β (TCRβ) repertoire in the CP and control groups. TCRβ sequencing revealed a significant increase in TCRβ repertoire diversity and reduced clonality in both CP groups versus controls. Interestingly, we observed differences in Vβ-Jβ gene family usage between hereditary and idiopathic CP and a positive correlation of TCRβ rearrangements with disease severity scores. Immunophenotyping analyses in hereditary and idiopathic CP pancreases indicate differences in innate and adaptive immune responses, which highlights differences in immunopathogenic mechanisms of disease among subtypes of CP. TCR repertoire analysis further suggests a role for specific T cell responses in hereditary versus idiopathic CP pathogenesis, providing insights into immune responses associated with human CP.

Authors

Bomi Lee, Julia Z. Adamska, Hong Namkoong, Melena D. Bellin, Josh Wilhelm, Gregory L. Szot, David M. Louis, Mark M. Davis, Stephen J. Pandol, Aida Habtezion

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Figure 3

TCRβ repertoire of control and CP pancreatic T cells.

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TCRβ repertoire of control and CP pancreatic T cells. (A) Waterfall and ...
(A) Waterfall and dot plots show the ratio of CD3+ T cell to CD68+ macrophage frequency in control, hereditary CP, and idiopathic CP tissues. Identified gene mutations are indicated in an individual hereditary CP patient. Mean ± SD; 1-way ANOVA with Tukey’s multiple-comparisons test. Her, hereditary. (B) One hundred most frequent rearrangements in each sample ranked from bottom (most frequent clone) to top (100th most frequent clone), and samples are listed by their clonality order from left to right. Number of productive rearrangements (C), TCR clonotype diversity (mean normalized Shannon-Wiener diversity index) (D), and productive clonality are shown (E). (CE) Comparison between control (n = 5) and CP (n = 13). Nonparametric Mann-Whitney U test. *P < 0.05, **P < 0.01.