RIG-E, a human homolog of the murine Ly-6 family, is induced by retinoic acid during the differentiation of acute promyelocytic leukemia cell.

Mao, Mao; Yu, Ming; Tong, Jianhua; Ye, Jing; Zhu, Jun; Huang, Qiu-Hua; Fu, Gang; Yu, Lingjia; Zhao, Shouyuan; Waxman, Samuel; Lanotte, Michel; Wang, Zhenyi; Tan, Jing-He; Chan, Sai-Juan; Chen, Zhu

doi:10.1073/pnas.93.12.5910

Cited by 99 publications

(67 citation statements)

References 23 publications

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“…46 Elucidation of the cascade of events leading to APL cell maturation by retinoids should benefit from the identification of RAR␣ targeted genes (primary targets), and also sets of genes that downstream are indirectly activated or repressed (secondary targets). Using a 'differential display' approach 47 we have identified new genes, RIG-E, 48 RIG-G, 49 and JEM-1, 50 that are modulated during retinoid-induced maturation of NB4 cells. These genes should serve as additional cell response markers; the elucidation of the mechanism of their transcriptional regulation should help to identify novel signalling pathways operating during APL cell maturation.…”

Section: Introductionmentioning

confidence: 99%

JEM-1, a novel nuclear co-factor: localisation and functional interaction with AP-1

Duprez

Lanotte

1999

Leukemia

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Section: Introductionmentioning

confidence: 99%

JEM-1, a novel nuclear co-factor: localisation and functional interaction with AP-1

Duprez

Lanotte

1999

Leukemia

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“…Certainly, CD59 homologues have been characterized in rabbit (14), rat (15), pig (16), and mouse (17). At the present time human homologues for several mouse Ly-6SF members are known, including ThB (18), Ly-6H (19), and TSA-1/Sca-2/RIG-E (20,21). In addition, the human urokinase plasminogen activator receptor (uPAR) consists of three Ly6SF domains (22,23).…”

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confidence: 99%

Ly-6I, a New Member of the Murine Ly-6 Superfamily with a Distinct Pattern of Expression

Pflugh

Maher

Bothwell

2000

The Journal of Immunology

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A new member of the mouse Ly-6SF, designated Ly-6I, has been isolated as a gene homologous to a segment of the Ly-6C gene. A single allelic difference in the mature protein sequence was identified, which is similar to other Ly-6SF members. Ly-6I mRNA has been detected in a wide range of tissues and cell lines, and a rabbit polyclonal Ab has been used to determine that Ly-6I protein is present at a low constitutive level on cell lines from several different lineages. In contrast to Ly-6C and Ly-6A/E, the Ly-6I gene is only weakly responsive to IFNs. Expression in vivo is most abundant on bone marrow populations and is coexpressed with Ly-6C on granulocytes and macrophages. However, Ly-6I is also expressed on immature B cell populations that do not express Ly-6C. Expression on mature B cells in spleen is uniformly low. Similarly, Ly-6I is expressed on TCRlow/int, but not TCRhigh, thymocytes. Ly-6I is re-expressed on Ly-6Chigh T cells in the periphery. Thus, Ly-6I may be a useful marker to define maturation stages of both T and B lymphocytes as well as subsets of monocytes and granulocytes.

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“…As a biological target, Ahr was best predicted by lymphocyte antigen 6e (Ly6e), a retinoic acid-responsive gene involved in T-cell activation (Mao et al 1996; Schedlich (Ahr,Cyp1b1,Lox,and Opn) are illustrated as described by Breitkreutz et al (2003) to identify focused gene networks regulated by the Ahr.…”

Section: Discussionmentioning

confidence: 99%

Unraveling gene-gene interactions regulated by ligands of the aryl hydrocarbon receptor

Johnson¹,

Balagurunathan²,

Tadesse³

et al. 2004

Environ. Health Perspect.

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RIG-E, a human homolog of the murine Ly-6 family, is induced by retinoic acid during the differentiation of acute promyelocytic leukemia cell.

Cited by 99 publications

References 23 publications

JEM-1, a novel nuclear co-factor: localisation and functional interaction with AP-1

JEM-1, a novel nuclear co-factor: localisation and functional interaction with AP-1

Ly-6I, a New Member of the Murine Ly-6 Superfamily with a Distinct Pattern of Expression

Unraveling gene-gene interactions regulated by ligands of the aryl hydrocarbon receptor

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