Transfer of in vivo primed transgenic T cells supports allergic lung inflammation and FIZZ1 and Ym1 production in an IL-4Rα and STAT6 dependent manner

Dasgupta, Preeta; Chapoval, Svetlana P; Smith, E. L.; Keegan, Achsah

doi:10.1186/1471-2172-12-60

Cited by 25 publications

(53 citation statements)

References 69 publications

(134 reference statements)

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“…RELMa is expressed by macrophages and pulmonary epithelial cells [2] and also by pulmonary vascular cells during hypoxia [1]. The Th-2 cytokines IL-4 and IL-13 induce RELMa expression via STAT6 and JAK-1 pathways [3,5]. RELMa has the capacity to promote lung cell proliferation, angiogenesis, and inflammation [1,6].…”

Section: Introductionmentioning

confidence: 99%

Resistin-Like Molecule α Stimulates Proliferation of Mesenchymal Stem Cells While Maintaining Their Multipotency

Kolosova

Angelini

Fan

et al. 2013

Stem Cells and Development

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Resistin-like molecule a (RELMa) is highly upregulated in the lungs of mice subjected to hypoxia. It is secreted from pulmonary epithelium and causes potent mitogenic, angiogenic, and vasoconstrictive effects in the lung vasculature. By using bone marrow transplantation in mice, we previously showed that RELMa is able to increase the number of bone marrow-derived cells in lung tissue, especially in the remodeling pulmonary vasculature. The current study investigated the effect of RELMa on progenitor stem cell content in mouse lung. Hypoxia, while stimulating RELMa expression, caused an increase in the number of Sca1 + /CD45 -progenitor cells in lungs of wild-type mice, but not in lungs of RELMa knockout mice. An in vitro study with cultured mesenchymal stem cells (MSCs) showed that RELMa induced a robust proliferative response that was dependent on Phosphatidylinositol 3-kinase/Akt and Erk activation. RELMa treatment of MSCs caused upregulation of a large number of genes involved in cell cycle, mitosis, organelle, and cytoskeleton biogenesis, and DNA metabolism. MSCs cultured in RELMa-supplemented media were able to maintain their differentiation potential into adipogenic, osteogenic, or mesenchymal phenotypes, although adipogenic differentiation was partially inhibited. These results demonstrate that RELMa may be involved in stem cell proliferation in the lung, without affecting differentiation potential.

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Section: Introductionmentioning

confidence: 99%

Resistin-Like Molecule α Stimulates Proliferation of Mesenchymal Stem Cells While Maintaining Their Multipotency

Kolosova

Angelini

Fan

et al. 2013

Stem Cells and Development

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“…Loss of STAT6 signaling caused a significant reduction in Retnla and Chi3L3 mRNA levels in bleomycin-induced lung fibrosis and allergic peritonitis models, respectively [27,28]. Using a murine model of asthma, we found that the number of AAMs recruited to the lungs in mice lacking STAT6 or IL-4Rα was much lower when compared to wild-type (WT) mice [29]. It has also been demonstrated that promoter regions of the Arg1 , Retnla and Chi3L3 genes have consensus STAT6-binding sites [28,30,31].…”

Section: Alternatively Activated Macrophagesmentioning

confidence: 99%

“…The contribution of FIZZ1 to asthma is still unclear. Our studies have shown that IL-4 induces robust induction of FIZZ1 mRNA in macrophages in vitro [25], but FIZZ1 protein expression in these cells was absent in vivo in a mouse model of asthma [29]. …”

Section: Specific Contribution Of Aam Products To Allergic Lung Inflamentioning

confidence: 99%

“…FIZZ1 was originally discovered in bronchoalveolar lavage fluid in a mouse model of asthma [77]. Elevated levels of FIZZ1 mRNA have since been detected in parasite infection models [69], allergic lung inflammation [28,29,77], allergic peritonitis [28], bleomycin-induced lung fibrosis [27] and hypoxia-induced pulmonary hypertension [78]. FIZZ1 has been reported to induce smooth muscle proliferation and actin and collagen deposition, causing fibrosis [79].…”

Section: Specific Contribution Of Aam Products To Allergic Lung Inflamentioning

confidence: 99%

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Contribution of Alternatively Activated Macrophages to Allergic Lung Inflammation: A Tale of Mice and Men

Dasgupta

Keegan

2012

J Innate Immun

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The concept that macrophages play an active role in inflammatory responses began its development in the late 1800s with the now iconic studies by Elie Metchnikoff using starfish larvae and Daphnia [reviewed in Kaufmann SHE: Nat Immunol 2008;9:705–712 and Cavaillon JM: J Leukoc Biol 2011;90:413–424]. Based on his observation of the phagocyte response to a foreign body (rose thorn) and yeast, he proposed that phagocytes acted in host defense and were active participants in the inflammatory process. Flash forward more than 100 years and we find that these basic tenets hold true. However, it is now appreciated that macrophages come in many different flavors and can adopt a variety of nuanced phenotypes depending on the tissue environment in which the macrophage is found. In this brief review, we discuss the role of one type of macrophage termed the alternatively activated macrophage (AAM), also known as the M2 type of macrophage, in regulating allergic lung inflammation and asthma. Recent studies using mouse models of allergic lung inflammation and samples from human asthma patients contribute to the emerging concept that AAMs are not just bystanders of the interleukin (IL)-4- and IL-13-rich environment found in allergic asthma but are also active players in orchestrating allergic lung disease.

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“…Previous work has shown that B cells from mice lacking STAT6 failed to produce significant amounts of IgE and IgG1 after infection with the nematode parasites (Raia et al, 2011;Turqueti-Neves et al, 2014). The binding sites of STAT6 have been found in the target regions of a variety of IL-4-mediated genes, including CD23 (Cooper et al, 2012), IL-4R (Jenkins et al, 2013), eotaxin-1 (Waddell et al, 2013), eotaxin-3 (Nakayama et al, 2010), FIZZ1 (Dasgupta et al, 2011), and in Ig germline e (Lu et al, 2007) promoters. Recently, IL-4-driven STAT6 constitutive activation has been found in various diseases, such as allergy (Hong et al, 2014), tumors (Cheah et al, 2014;Creytens et al, in press;Koelsche et al, 2014), and lymphoproliferative disorders (Rawal et al, 2013).…”

Section: Introductionmentioning

confidence: 99%

Histone H3k9 and H3k27 Acetylation Regulates IL‐4/STAT6‐Mediated Igε Transcription in B Lymphocytes

Wang

Duan

et al. 2015

The Anatomical Record

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IL-4 activates STAT6 and causes the subsequent up-regulation of Ig heavy chain germline Ige via chromatin remodeling involved in B lymphocytes development. STAT6 acts as a molecular switch to regulate the higher-order chromatin remodeling via dynamically orchestrating co-activators (CBP/Tudor-SN) and co-repressors (HDAC1/PSF). Here, we demonstrated that STAT6/Tudor-SN/PSF form a complex, balancing the acetylation and deacetylation states to co-regulate IL-4/STAT6 gene transcription. In addition, we confirmed that IL-4 treatment increased the HATs activity in Ramos cells. As "active" markers, the expression of H3K9ac and H3K27ac increased after treatment with IL-4. However, transcriptional repressors such as H3K9me3 and H3K27me3 decreased in response to IL-4 stimulation. Moreover, IL-4 treatment enhanced H3 acetylation at the Ige promoter regions. Our results revealed that the Ige gene transcription is regulated by histone modifications in the IL-4/STAT6 pathway. The study will provide novel insights into the pathogenesis of allergic diseases.

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Transfer of in vivo primed transgenic T cells supports allergic lung inflammation and FIZZ1 and Ym1 production in an IL-4Rα and STAT6 dependent manner

Cited by 25 publications

References 69 publications

Resistin-Like Molecule α Stimulates Proliferation of Mesenchymal Stem Cells While Maintaining Their Multipotency

Resistin-Like Molecule α Stimulates Proliferation of Mesenchymal Stem Cells While Maintaining Their Multipotency

Contribution of Alternatively Activated Macrophages to Allergic Lung Inflammation: A Tale of Mice and Men

Histone H3k9 and H3k27 Acetylation Regulates IL‐4/STAT6‐Mediated Igε Transcription in B Lymphocytes

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