Literature DB >> 12819012

Molecular characterization of NF-HEV, a nuclear factor preferentially expressed in human high endothelial venules.

Espen S Baekkevold1, Myriam Roussigné, Takeshi Yamanaka, Finn-Eirik Johansen, Frode L Jahnsen, François Amalric, Per Brandtzaeg, Monique Erard, Guttorm Haraldsen, Jean-Philippe Girard.   

Abstract

Lymphocyte homing to secondary lymphoid tissue and lesions of chronic inflammation is directed by multi-step interactions between the circulating cells and the specialized endothelium of high endothelial venules (HEVs). In this study, we used the PCR-based method of suppression subtractive hybridization (SSH) to identify novel HEV genes by comparing freshly purified HEV endothelial cells (HEVECs) with nasal polyp-derived microvascular endothelial cells (PMECs). By this approach, we cloned the first nuclear factor preferentially expressed in HEVECs, designated nuclear factor from HEVs (NF-HEV). Virtual Northern and Western blot analyses showed strong expression of NF-HEV in HEVECs, compared to human umbilical vein endothelial cells (HUVECs) and PMECs. In situ hybridization and immunohistochemistry revealed that NF-HEV mRNA and protein are expressed at high levels and rather selectively by HEVECs in human tonsils, Peyers's patches, and lymph nodes. The NF-HEV protein was found to contain a bipartite nuclear localization signal, and was targeted to the nucleus when ectopically expressed in HUVECs and HeLa cells. Furthermore, endogenous NF-HEV was found in situ to be confined to the nucleus of tonsillar HEVECs. Finally, threading and molecular modeling studies suggested that the amino-terminal part of NF-HEV (aa 1-60) corresponds to a novel homeodomain-like Helix-Turn-Helix (HTH) DNA-binding domain. Similarly to the atypical homeodomain transcription factor Prox-1, which plays a critical role in the induction of the lymphatic endothelium phenotype, NF-HEV may be one of the key nuclear factors that controls the specialized HEV phenotype.

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Year:  2003        PMID: 12819012      PMCID: PMC1868188          DOI: 10.1016/S0002-9440(10)63631-0

Source DB:  PubMed          Journal:  Am J Pathol        ISSN: 0002-9440            Impact factor:   4.307


  51 in total

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Journal:  Nucleic Acids Res       Date:  1997-07-01       Impact factor: 16.971

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Journal:  Am J Pathol       Date:  1997-06       Impact factor: 4.307

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Journal:  Am J Pathol       Date:  1999-10       Impact factor: 4.307

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  165 in total

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Review 2.  Research progress on interleukin-33 and its roles in the central nervous system.

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4.  IL-33 is processed into mature bioactive forms by neutrophil elastase and cathepsin G.

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Journal:  Proc Natl Acad Sci U S A       Date:  2012-01-17       Impact factor: 11.205

5.  Murine mast cells secrete and respond to interleukin-33.

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Journal:  J Interferon Cytokine Res       Date:  2013-09-12       Impact factor: 2.607

6.  Contradictory functions (activation/termination) of neutrophil proteinase 3 enzyme (PR3) in interleukin-33 biological activity.

Authors:  Suyoung Bae; Taebong Kang; Jaewoo Hong; Siyoung Lee; Jida Choi; Hyunjhung Jhun; Areum Kwak; Kwangwon Hong; Eunsom Kim; Seunghyun Jo; Soohyun Kim
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7.  Interleukin-33 in the human placenta.

Authors:  Vanessa Topping; Roberto Romero; Nandor Gabor Than; Adi L Tarca; Zhonghui Xu; Sun Young Kim; Bing Wang; Lami Yeo; Chong Jai Kim; Sonia S Hassan; Jung-Sun Kim
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8.  Serum amyloid A induces interleukin-33 expression through an IRF7-dependent pathway.

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Journal:  Eur J Immunol       Date:  2014-05-22       Impact factor: 5.532

9.  Human basophils and eosinophils are the direct target leukocytes of the novel IL-1 family member IL-33.

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Journal:  Blood       Date:  2008-10-27       Impact factor: 22.113

Review 10.  Disease-associated functions of IL-33: the new kid in the IL-1 family.

Authors:  Foo Y Liew; Nick I Pitman; Iain B McInnes
Journal:  Nat Rev Immunol       Date:  2010-01-18       Impact factor: 53.106

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