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51. Design and Characterization of Superpotent Bivalent Ligands Targeting Oxytocin Receptor Dimers via a Channel-Like Structure

54. Synthesis of Multivalent [Lys8]-Oxytocin Dendrimers that Inhibit Visceral Nociceptive Responses.

56. Selenoether oxytocin analogues have analgesic properties in a mouse model of chronic abdominal pain

57. α-conotoxin AuIB isomers exhibit distinct inhibitory mechanisms and differential sensitivity to stoichiometry of α3β4 nicotinic acetylcholine receptors

58. Solving the α-conotoxin folding problem: efficient selenium-directed on-resin generation of more potent and stable nicotinic acetylcholine receptor antaqonists

68. Solving the α-Conotoxin Folding Problem: Efficient Selenium-Directed On-Resin Generation of More Potent and Stable Nicotinic Acetylcholine Receptor Antagonists

72. Site‐Specific pKaDetermination of Selenocysteine Residues in Selenovasopressin by Using 77Se NMR Spectroscopy

73. p-Nitrobenzyl protection for cysteine and selenocysteine: A more stable alternative to the acetamidomethyl group

74. Development of a human vasopressin V1a-receptor antagonist from an evolutionary-related insect neuropeptide.

76. Validacija antitijela za OTR i V1aR pristupima temeljenima na proteomici

77. Oxytocin Analogues for the Oral Treatment of Abdominal Pain.

78. Intestinal biofilms: pathophysiological relevance, host defense, and therapeutic opportunities.

79. Novel Diacyl-hydrazide Compounds as Potential Therapeutics for Visceral Leishmaniasis.

80. Archaea influence composition of endoscopically visible ileocolonic biofilms.

81. Fmoc Solid Phase Peptide Synthesis of Oxytocin and Analogues.

82. Anhydrous Hydrogen Fluoride Cleavage in Boc Solid Phase Peptide Synthesis.

83. Advancing the Frontiers of Chemical Protein Synthesis-The 7 th CPS Meeting, Haifa, Israel.

84. Alpha-conotoxin AuIB isomers exhibit distinct inhibitory mechanisms and differential sensitivity to stoichiometry of alpha3beta4 nicotinic acetylcholine receptors.

85. Ligand-based peptide design and combinatorial peptide libraries to target G protein-coupled receptors.

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