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Start Over You searched for: Author "Hudig D" Remove constraint Author: "Hudig D" Topic t-lymphocytes, cytotoxic Remove constraint Topic: t-lymphocytes, cytotoxic
16 results on '"Hudig D"'

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1. Pancreatic lipase-related protein 2 (PLRP2) induction by IL-4 in cytotoxic T lymphocytes (CTLs) and reevaluation of the negative effects of its gene ablation on cytotoxicity.

2. Lipid-dependent cytotoxicity by the lipase PLRP2 and by PLRP2-positive cytotoxic T lymphocytes (CTLs).

3. Hydrolysis of tumor cell lipids after CTL-mediated death.

4. Regulation of perforin lysis: implications for protein disulfide isomerase proteins.

5. Granzymes (lymphocyte serine proteases): characterization with natural and synthetic substrates and inhibitors.

6. Interaction between a Ca2+-binding protein calreticulin and perforin, a component of the cytotoxic T-cell granules.

7. P-4 and RNKP-7, new granzyme-like serine proteases expressed in activated rat lymphocytes.

8. Fractionation of perforin and granzymes by immobilized metal affinity chromatography (IMAC).

9. Characterization, application and potential uses of biotin-tagged inhibitors for lymphocyte serine proteases (granzymes).

10. Binding of granzyme B in the nucleus of target cells. Recognition of an 80-kilodalton protein.

11. Activation of recombinant murine cytotoxic cell proteinase-1 requires deletion of an amino-terminal dipeptide.

12. RNKP-1, a novel natural killer-associated serine protease gene cloned from RNK-16 cytotoxic lymphocytes.

13. Localization, implications for function, and gene expression of chymotrypsin-like proteinases of cytotoxic RNK-16 lymphocytes.

14. The mechanism of cell-mediated cytotoxicity. III. Protease-specific inhibitors preferentially block later events in cytotoxic T lymphocyte-mediated lysis than do inhibitors of methylation or thiol-reactive agents.

15. The mechanism of cell-mediated cytotoxicity. IV. K-76 COONa, which inhibits the activity of Factor I and of C5, inhibits early events in cytotoxic T-lymphocyte-mediated cytolysis and in T-lymphocyte activation.

16. Cell surface thiols, methylation, and complement-like components are involved in the early events of CML whereas proteases participate in the later, Ca++-dependent events.

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