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1. Chemokine Receptor N-Terminus Charge Dictates Reliance on Post-Translational Modifications for Effective Ligand Capture and Following Boosting by Defense Peptides.

2. Altered O-glycosylation of β 1 -adrenergic receptor N-terminal single-nucleotide variants modulates receptor processing and functional activity.

3. "Glyco-sulfo barcodes" regulate chemokine receptor function.

4. GPR37 is processed in the N-terminal ectodomain by ADAM10 and furin.

5. The N-terminal domain of unknown function (DUF959) in collagen XVIII is intrinsically disordered and highly O-glycosylated.

6. Site-specific O-glycosylation of N-terminal serine residues by polypeptide GalNAc-transferase 2 modulates human δ-opioid receptor turnover at the plasma membrane.

7. Site-specific O -Glycosylation by Polypeptide N -Acetylgalactosaminyltransferase 2 (GalNAc-transferase T2) Co-regulates β 1 -Adrenergic Receptor N-terminal Cleavage.

8. N-Glycan-dependent and -independent quality control of human δ opioid receptor N-terminal variants.

9. Targeting opioid receptors with pharmacological chaperones.

10. β-Adrenergic agonists mediate enhancement of β1-adrenergic receptor N-terminal cleavage and stabilization in vivo and in vitro.

11. Cys-27 variant of human δ-opioid receptor modulates maturation and cell surface delivery of Phe-27 variant via heteromerization.

12. Cysteine 27 variant of the delta-opioid receptor affects amyloid precursor protein processing through altered endocytic trafficking.

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