Rebecca P. Schall scite author profile

We previously isolated a series of cDNA clones designated NKG2-A, B, C, and D from a human natural killer (NK) cell library. These transcripts encode a family of type II integral membrane proteins having an extracellular Ca(2+)-dependent lectin domain. The predicted peptides share structural similarities and amino acid sequence similarity with known receptor molecules. In this report, the genomic organization and mRNA expression of each of the genes were studied by using transcript-specific probes. Southern blot experiments reveal that the probes cross-hybridize with a maximum of five genes at high stringency. By probing a Southern blot prepared from a series of hamster/human hybrid somatic cell lines, we demonstrated that all of the hybridizing fragments occur on human chromosome 12. No gene rearrangement and little restriction fragment length polymorphism (RFLP) was observed with these probes. mRNA expression of the NKG2 genes occurred in NK cells and some T cells but not in other hematopoietic cell types or in other tissues tested. Each of the transcripts occurred in all three of the NK cell lines tested: however, the genes were differentially regulated in T cells. NKG2-D was expressed in nine of fourteen T-cell clones or lines in the panel, whereas NKG2-A/B was expressed in three and NKG2-C was expressed in only one. Expression of each of the transcripts was upregulated following T-cell growth factor (TCGF)-induced activation of a cloned NK cell. The limited distribution of these proteins and their sequence similarity with known receptor molecules suggest that they may function as receptors on human NK cells.

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Difluoromethylornithine (DFMO) arrests murine CTL development in the late, pre-effector stage

Schall¹,

Sekar²,

Tandon³

et al. 1991

Immunopharmacology

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Identification of a novel gene expressed in activated natural killer cells and T cells.

Dahl

Schall

et al. 1992

182

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We have isolated a cDNA clone from a human activated NK cell-derived cDNA library that identifies a transcript (NK4) that is selectively expressed in lymphocytes. The expression of this transcript is increased after activation of T cells by mitogens or activation of NK cells by IL-2 (lymphokine-activated killer cells). The transcript levels demonstrated by Northern blot analysis increase by 12 h after activation, remain high for at least 48 h, and require protein synthesis for expression. Southern blot analysis of B lymphoblastoid lines derived from 18 unrelated individuals reveal variable banding patterns suggestive of polymorphism within the NK4 gene. No homology was found between the sequence of the coding region of this transcript and any sequences in the GenBank data base. Sequence homology to the U1 small nuclear RNA was found within the 3' untranslated region immediately upstream of the site of polyadenylation, suggesting a possible role for U1 in the polyadenylation process. Sequence analysis indicates the transcript would encode a protein having a mass of 27 kDa. The presence of a signal sequence and lack of a transmembrane region suggests that the protein is secreted. In addition, the protein contains an RGD sequence that may be involved in cellular adhesion. This transcript appears to encode a novel product common to the activation pathways of both NK cells and T cells.

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A monoclonal antibody (RH1-38) which inhibits multiple systems of cell-mediated cytotoxicity—II. Evidence that the epitope recognized is involved in a late step in the cytolytic mechanism

Hall

Schall

Black

1985

Molecular Immunology

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Regulatory mechanisms in cytotoxic T lymphocyte development

Süßkind

Schall

Dixon

1986

Cellular Immunology

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Rebecca P. Schall

A multigene family on human chromosome 12 encodes natural killer-cell lectins

Difluoromethylornithine (DFMO) arrests murine CTL development in the late, pre-effector stage

Identification of a novel gene expressed in activated natural killer cells and T cells.

A monoclonal antibody (RH1-38) which inhibits multiple systems of cell-mediated cytotoxicity—II. Evidence that the epitope recognized is involved in a late step in the cytolytic mechanism

Regulatory mechanisms in cytotoxic T lymphocyte development

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