Schlafen 4–expressing myeloid-derived suppressor cells are induced during murine gastric metaplasia

Ding, Lin; Hayes, Michael M.; Photenhauer, Amanda; Eaton, Kathryn A.; Li, Qian; Ocadiz-Ruiz, Ramon; Merchant, Juanita L.

doi:10.1172/jci82529

Cited by 63 publications

(99 citation statements)

References 54 publications

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“…A study by the Merchant laboratory identified Schlafen 4 ( Slfn4 ) as a GLI1 target gene and myeloid differentiation factor that correlated with the development of SPEM in mice 77 . A recent study by the same group then showed that migration of Slfn4-expressing cells from the bone marrow to the stomach in response to Helicobacter infection showed MDSC markers, and acquired the ability to inhibit T-cell proliferation 78 . This supports MDSC suppression of T-cell function and subsequent dampening of the immune response to create a microenvironment favoring tumor growth 79 …”

Section: Maintenance Of Gastric Cancer: the Role Of The Cancer Stem Cmentioning

confidence: 99%

Initiation and Maintenance of Gastric Cancer: A Focus on CD44 Variant Isoforms and Cancer Stem Cells

Zavros

2017

Cellular and Molecular Gastroenterology and Hepatology

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Gastric cancer is the third most common cause of cancer-related death. Although the incidence of gastric cancer in the United States is relatively low, it remains significantly higher in some countries, including Japan and Korea. Interactions between cancer stem cells and the tumor microenvironment can have a substantial impact on tumor characteristics and contribute to heterogeneity. The mechanisms responsible for maintaining malignant cancer stem cells within the tumor microenvironment in human gastric cancer are largely unknown. Tumor cell and genetic heterogeneity contribute to either de novo intrinsic or the therapy-induced emergence of drug-resistant clones and eventual tumor recurrence. Although chemotherapy often is capable of inducing cell death in tumors, many cancer patients experience recurrence because of failure to effectively target the cancer stem cells, which are believed to be key tumor-initiating cells. Among the population of stem cells within the stomach that may be targeted during chronic Helicobacter pylori infection and altered into tumor-initiating cells are those cells marked by the cluster-of-differentiation (CD)44 cell surface receptor. CD44 variable isoforms (CD44v) have been implicated as key players in malignant transformation whereby their expression is highly restricted and specific, unlike the canonical CD44 standard isoform. Overall, CD44v, in particular CD44v9, are believed to mark the gastric cancer cells that contribute to increased resistance for chemotherapy- or radiation-induced cell death. This review focuses on the following: the alteration of the gastric stem cell during bacterial infection, and the role of CD44v in the initiation, maintenance, and growth of tumors associated with gastric cancer.

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Section: Maintenance Of Gastric Cancer: the Role Of The Cancer Stem Cmentioning

confidence: 99%

Initiation and Maintenance of Gastric Cancer: A Focus on CD44 Variant Isoforms and Cancer Stem Cells

Zavros

2017

Cellular and Molecular Gastroenterology and Hepatology

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“…All mouse experiments were approved by the University of Michigan’s Institutional Animal Care and Use Committee. Transgenic Shh mice (promoter for cytomegalovirus [pCVM]‐ Shh ) and Gli1 lacZ/lacZ mice have been described . The Gli1 lacZ./+ and Gli1 lacZ./lacZ mice contain a knock‐in lacZ , encoding a nuclear‐localized β‐galactosidase, into exon 2 of the mouse Gli1 gene, producing a null allele .…”

Section: Methodsmentioning

confidence: 99%

“…HH signaling involves Sonic hedgehog (SHH) and Indian hedgehog (IHH) ligands, the receptor Patched‐1 (PTCH1), and their transcriptional effectors glioma‐associated oncogene 1 (GLI1), GLI2, and GLI3 . In the canonical HH pathway, cells expressing HH ligand signal to stromal cells expressing PTCH1 and GLIs in a variety of gastrointestinal tissues . In the liver, HH ligands are expressed in both epithelial cells and myofibroblasts after injury, and HH signaling is responsible for the “reactive” phenotype of injured cholangiocytes .…”

mentioning

confidence: 99%

“…(1) In the canonical HH pathway, cells expressing HH ligand signal to stromal cells expressing PTCH1 and GLIs in a variety of gastrointestinal tissues. (2)(3)(4) In the liver, HH ligands are expressed in both epithelial cells and myofibroblasts after injury, and HH signaling is responsible for the "reactive" phenotype of injured cholangiocytes. (5,6) Prior studies, including from our group, suggest that HH signaling contributes to the initiation and progression of cholangiocarcinoma.…”

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confidence: 99%

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Hedgehog Signaling Modulates Interleukin‐33‐Dependent Extrahepatic Bile Duct Cell Proliferation in Mice

et al. 2018

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Hedgehog (HH) signaling participates in hepatobiliary repair after injury and is activated in patients with cholangiopathies. Cholangiopathies are associated with bile duct (BD) hyperplasia, including expansion of peribiliary glands, the niche for biliary progenitor cells. The inflammation‐associated cytokine interleukin (IL)‐33 is also up‐regulated in cholangiopathies, including cholangiocarcinoma. We hypothesized that HH signaling synergizes with IL‐33 in acute inflammation‐induced BD hyperplasia. We measured extrahepatic BD (EHBD) thickness and cell proliferation with and without an IL‐33 challenge in wild‐type mice, mice overexpressing Sonic HH (pCMV‐Shh), and mice with loss of the HH pathway effector glioma‐associated oncogene 1 (Gli1lacZ/lacZ). LacZ reporter mice were used to map the expression of HH effector genes in mouse EHBDs. An EHBD organoid (BDO) system was developed to study biliary progenitor cells in vitro. EHBDs from the HH overexpressing pCMV‐Shh mice showed increased epithelial cell proliferation and hyperplasia when challenged with IL‐33. In Gli1lacZ/lacZ mice, we observed a decreased proliferative response to IL‐33 and decreased expression of Il6. The HH ligands Shh and Indian HH (Ihh) were expressed in epithelial cells, whereas the transcriptional effectors Gli1, Gli2, and Gli3 and the HH receptor Patched1 (Ptch1) were expressed in stromal cells, as assessed by in situ hybridization and lacZ reporter mice. Although BDO cells lacked canonical HH signaling, they expressed the IL‐33 receptor suppression of tumorigenicity 2. Accordingly, IL‐33 treatment directly induced BDO cell proliferation in a nuclear factor κB‐dependent manner. Conclusion: HH ligand overexpression enhances EHBD epithelial cell proliferation induced by IL‐33. This proproliferative synergism of HH and IL‐33 involves crosstalk between HH ligand‐producing epithelial cells and HH‐responding stromal cells.

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“…Myeloid cell polarization into MDSCs requires hedgehog-regulated transcription factor GLI1, which induces gastric MDSCs to express Schlafen 4 , a myeloid differentiation factor. 79 Dr Merchant showed that a nucleic acid signature for MDSCs in plasma correlates with gastric metaplasia presence in both mice and humans. Collectively, her studies suggest that MDSCs are present in the gastric microenvironment before neoplastic transformation, and that they might serve as a biomarker for gastric cancer risk.…”

Section: Inflammation and The Development Of Metaplasia Sessionmentioning

confidence: 99%

A Summary of the 2016 James W. Freston Conference of the American Gastroenterological Association: Intestinal Metaplasia in the Esophagus and Stomach: Origins, Differences, Similarities and Significance

et al. 2017

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Schlafen 4–expressing myeloid-derived suppressor cells are induced during murine gastric metaplasia

Cited by 63 publications

References 54 publications

Initiation and Maintenance of Gastric Cancer: A Focus on CD44 Variant Isoforms and Cancer Stem Cells

Initiation and Maintenance of Gastric Cancer: A Focus on CD44 Variant Isoforms and Cancer Stem Cells

Hedgehog Signaling Modulates Interleukin‐33‐Dependent Extrahepatic Bile Duct Cell Proliferation in Mice

A Summary of the 2016 James W. Freston Conference of the American Gastroenterological Association: Intestinal Metaplasia in the Esophagus and Stomach: Origins, Differences, Similarities and Significance

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