Progressive loss of endothelial P-selectin expression with increasing malignancy in colorectal cancer

BALB/c mice develop aberrant T helper 2 (Th2) responses and suffer progressive disease after infection with Leishmania major. These outcomes depend on the production of interleukin-4 (IL-4) early after infection. Here we demonstrate that the burst of IL-4 mRNA, peaking in draining lymph nodes of BALB/c mice 16 hr after infection, occurs within CD4+ T cells that express V beta 4 V alpha 8 T cell receptors. In contrast to control and V beta 6-deficient BALB/c mice, V beta 4-deficient BALB/c mice were resistant to infection, demonstrating the role of these cells in Th2 development. The early IL-4 response was absent in these mice, and T helper 1 responses occurred following infection. Recombinant LACK antigen from L. major induced comparable IL-4 production in V beta 4 V alpha 8 CD4+ cells. Thus, the IL-4 required for Th2 development and susceptibility to L. major is produced by a restricted population of V beta 4 V alpha 8 CD4+ T cells after cognate interaction with a single antigen from this complex organism.

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Generation of avian myeloblastosis virus structural proteins by proteolytic cleavage of a precursor polypeptide

Vogt

Eisenman

Diggelmann

1975

Journal of Molecular Biology

295

138

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Clonal deletion of V β814-bearing T cells in mice transgenic for mammary tumour virus

Acha‐Orbea

Shakhov²,

Scarpellino

et al. 1991

Nature

272

129

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Autoreactive T lymphocytes are clonally deleted during maturation in the thymus. Deletion of T cells expressing particular receptor V beta elements is controlled by poorly defined autosomal dominant genes. A gene has now been identified by expression of transgenes in mice which causes deletion of V beta 14+ T cells. The gene lies in the open reading frame of the long terminal repeat of the mouse mammary tumour virus.

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Hygromycin B phosphotransferase as a selectable marker for DNA transfer experiments with higher eucaryotic cells.

Blöchlinger¹,

Diggelmann²

1984

Mol. Cell. Biol.

254

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The DNA coding sequence for the hygromycin B phosphotransferase gene was placed under the control of the regulatory sequences of a cloned long terminal repeat of Moloney sarcoma virus. This construction allowed direct selection for hygromycin B resistance after transfection of eucaryotic cell lines not naturally resistant to this antibiotic, thus providing another dominant marker for DNA transfer in eucaryotic cells.

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Glucocorticoid regulation of mouse mammary tumor virus: identification of a short essential DNA region.

Buetti¹,

Diggelmann²

1983

The EMBO Journal

119

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Transcription of mouse mammary tumor virus (MMTV) DNA is stimulated by steroid hormones. To determine the DNA sequences involved in this regulation, we constructed a plasmid containing the MMTV long terminal repeat (LTR) in front of the coding region of the herpes simplex thymidine kinase gene, from which the promoter had been removed. Portions of the LTR were removed by the nuclease Ba/31, and the deleted molecules were recloned and tested for transcriptional activity in transfections of Ltk‐aprt‐ cells. Stably transfected cell clones were selected and hormone‐dependent transcription from the MMTV promoter was studied by the S1 nuclease mapping method. The results show that DNA sequences between ‐105 and ‐204 base pairs upstream from the initiation site of viral transcription are required for glucocorticoid stimulation.

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Cloned mouse mammary tumor virus DNA is biologically active in transfected mouse cells and its expression is stimulated by glucocorticoid hormones

Buetti

Diggelmann

1981

Cell

171

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The region of mouse mammary tumor virus DNA containing the long terminal repeat includes a long coding sequence and signals for hormonally regulated transcription.

Fasel¹,

Pearson²,

Buetti³

et al. 1982

The EMBO Journal

153

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Starting from a biologically active recombinant DNA clone of exogenous unintegrated GR mouse mammary tumor virus, we have generated three subclones of PstI fragments of 1.45, 1.1, and 2.0 kb in the plasmid vector PBR322. The nucleotide sequence has been determined for the clone of 1.45 kb which includes almost the complete region of the long terminal repeat (LTR) plus an adjacent stretch of unique sequence DNA. A short region of the 2.0 kb clone, containing the beginning of the LTR, has also been sequenced. Starting with the A of an initiation codon outside the LTR, we detected an open reading frame of 960 nucleotides, potentially coding for a protein of 320 amino acids (36K). Two hundred nucleotides downstream from the termination codon, and approximately 25 nucleotides upstream from the presumptive initiation site of viral RNA synthesis, we found a promoter‐like sequence. The sequence AGTAAA was detected approximately 15‐20 nucleotides upstream from the 3′ end of virion RNA and probably serves as a polyadenylation signal. The 1.45 kb PstI fragment has been transfected into Ltk‐ cells together with a plasmid containing the thymidine kinase gene of herpes simplex virus. The virus‐specific RNA synthesis detected in a Tk+ cell clone was strongly stimulated by the addition of dexamethasone.

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Gene transfer into stimulated and unstimulated T lymphocytes by HIV-1-derived lentiviral vectors

et al. 2000

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Heidi Diggelmann

IL-4 Rapidly Produced by Vβ4 Vα8 CD4+ T Cells Instructs Th2 Development and Susceptibility to Leishmania major in BALB/c Mice

Generation of avian myeloblastosis virus structural proteins by proteolytic cleavage of a precursor polypeptide

Clonal deletion of V β814-bearing T cells in mice transgenic for mammary tumour virus

Hygromycin B phosphotransferase as a selectable marker for DNA transfer experiments with higher eucaryotic cells.

Glucocorticoid regulation of mouse mammary tumor virus: identification of a short essential DNA region.

Cloned mouse mammary tumor virus DNA is biologically active in transfected mouse cells and its expression is stimulated by glucocorticoid hormones

The region of mouse mammary tumor virus DNA containing the long terminal repeat includes a long coding sequence and signals for hormonally regulated transcription.

Gene transfer into stimulated and unstimulated T lymphocytes by HIV-1-derived lentiviral vectors

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