The Presence of Interleukin-13 at Pancreatic ADM/PanIN Lesions Alters Macrophage Populations and Mediates Pancreatic Tumorigenesis

Liou, Geou-Yarh; Bastea, Ligia I.; Fleming, Alicia K.; Döppler, Heike; Edenfield, Brandy; Dawson, David W.; Zhang, Lizhi; Bardeesy, Nabeel; Störz, Peter

doi:10.1016/j.celrep.2017.04.052

Cited by 88 publications

(126 citation statements)

References 36 publications

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“…Recently, in a KRAS model of PDA, tumor-associated macrophages increased with ductal metaplasia and neoplastic transformation, effects that appeared to depend on IL-13 released from cancer cells. 47 On the other hand, several pathways have been proposed to mediate the effects of tumor-associated macrophages on cancerous epithelium. 10,13,29 Here we found that expression of PEDF, a tumor suppressor in PDA, decreases in the transforming epithelium not due to KRAS mutation but upon exposure to macrophages.…”

Section: Discussionmentioning

confidence: 99%

KRAS mutation and epithelial–macrophage interplay in pancreatic neoplastic transformation

Bishehsari

Zhang

Barlass

et al. 2018

Intl Journal of Cancer

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Pancreatic ductal adenocarcinoma (PDA) is characterized by epithelial mutations in KRAS and prominent tumor-associated inflammation, including macrophage infiltration. But knowledge of early interactions between neoplastic epithelium and macrophages in PDA carcinogenesis is limited. Using a pancreatic organoid model, we found that the expression of mutant KRAS in organoids increased (i) ductal to acinar gene expression ratios, (ii) epithelial cells proliferation and (iii) colony formation capacity in vitro, and endowed pancreatic cells with the ability to generate neoplastic tumors in vivo. KRAS mutations induced a protumorigenic phenotype in macrophages. Altered macrophages decreased epithelial pigment epithelial derived factor (PEDF) expression and induced a cancerous phenotype. We validated our findings using annotated patient samples from The Cancer Genome Atlas (TCGA) and in our human PDA specimens. Epithelium-macrophage cross-talk occurs early in pancreatic carcinogenesis where KRAS directly induces cancer-related phenotypes in epithelium, and also promotes a protumorigenic phenotype in macrophages, in turn augmenting neoplastic growth.

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Section: Discussionmentioning

confidence: 99%

KRAS mutation and epithelial–macrophage interplay in pancreatic neoplastic transformation

Bishehsari

Zhang

Barlass

et al. 2018

Intl Journal of Cancer

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“…Enrichment of DCLK1 and acetylated α-tubulin in the FACS-sorted CD133 + population of PDAC cells was reported (Bailey et al, 2014). Expression of CD133, DCLK1 and CD44 were present in PanIN cells of oncogenic Kras G12D mouse pancreas (Fig 2, (Bailey et al, 2014, Delgiorno et al, 2014, Liou et al, 2017)). However, these 3 CSC markers were expressed in different subpopulations of murine PanIN cells (Fig 2.…”

Section: Cd133 In Cancer Development and Progressionmentioning

confidence: 91%

CD133 as a regulator of cancer metastasis through the cancer stem cells

Liou

2019

The International Journal of Biochemistry & Cell Biology

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Cancer stem cells are the cancer cells that have abilities to self-renew, differentiate into defined progenies, and initiate and maintain tumor growth. They also contribute to cancer metastasis and therapeutic resistance, both of which are the major causes of cancer mortality. Among the reported makers of the cancer stem cells, CD133 is the most well-known marker for isolating and studying cancer stem cells in different types of cancer. The CD133high population of cancer cells are not only capable of self-renewal, proliferation, but also highly metastatic and resistant to therapy. Despite very limited information on physiological functions of CD133, many ongoing studies are aimed to reveal the mechanisms that CD133 utilizes to modulate cancer dissemination and drug resistance with a long-term goal for bringing down the number of cancer deaths. In this review, in addition to the regulation of CD133, and its involvement in cancer initiation, and development, the recent updates on how CD133 modulates cancer dissemination, and therapeutic resistance are provided. The key signaling pathways that are upstream or downstream of CD133 during these processes are summarized. A comprehensive understanding of CD133-mediated cancer initiation, development, and dissemination through its pivotal role in cancer stem cells will offer new strategies in cancer therapy.

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“…Macrophage-secreted inflammatory cytokines, such as tumour necrosis factor (TNF) and CC motif chemokine 5 (CCL5), play roles in pancreatic ADM, with contributions from macrophage-released matrix metalloproteinases (MMPs), such as MMP9, as well 131,132 . Recently, it was demonstrated that IL-13 alters macrophage populations from an inflammatory macrophage subpopulation to an alternatively activated macrophage subpopulation in ADM 133 . The development of Barrett-like metaplasia in the mouse requires the suppression of CD8 + T cell-dependent apoptosis of epithelial cells, which is probably mediated by CD11b + GR1 + immature myeloid cells or myeloid-derived suppressor cells 134 .…”

Section: Epigenetic and Genomic Considerationsmentioning

confidence: 99%

Metaplasia: tissue injury adaptation and a precursor to the dysplasia–cancer sequence

2017

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Metaplasia is the replacement of one differentiated somatic cell type with another differentiated somatic cell type in the same tissue. Typically, metaplasia is triggered by environmental stimuli, which may act in concert with the deleterious effects of microorganisms and inflammation. The cell of origin for intestinal metaplasia in the oesophagus and stomach and for pancreatic acinar–ductal metaplasia has been posited through genetic mouse models and lineage tracing but has not been identified in other types of metaplasia, such as squamous metaplasia. A hallmark of metaplasia is a change in cellular identity, and this process can be regulated by transcription factors that initiate and/or maintain cellular identity, perhaps in concert with epigenetic reprogramming. Universally, metaplasia is a precursor to low-grade dysplasia, which can culminate in high-grade dysplasia and carcinoma. Improved clinical screening for and surveillance of metaplasia might lead to better prevention or early detection of dysplasia and cancer.

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The Presence of Interleukin-13 at Pancreatic ADM/PanIN Lesions Alters Macrophage Populations and Mediates Pancreatic Tumorigenesis

Cited by 88 publications

References 36 publications

KRAS mutation and epithelial–macrophage interplay in pancreatic neoplastic transformation

KRAS mutation and epithelial–macrophage interplay in pancreatic neoplastic transformation

CD133 as a regulator of cancer metastasis through the cancer stem cells

Metaplasia: tissue injury adaptation and a precursor to the dysplasia–cancer sequence

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