Deamino- and Decarboxy-Histidine Derivatives

Deamino- and Decarboxy-Histidine Derivatives

Published on 10/11/2020

Interested in histidine derivatives? Iris Biotech provides a selection of deamino- and decarboxy-products. Find out more about benefits and potential applications of our new building blocks.

Deamino- and Decarboxy-Histidine Derivatives

The essential amino acid Histidine (His, H), first isolated in 1896 by Albrecht Kossel and Sven Gustaf Hedin, bears an imidazole side chain which plays a crucial role for the activity of many enzymes. It can act as a proton shuttle and with its two N-donors it is one of the most effective ligation sites in metallopeptides.

An example for an essential histidine-bearing peptide is the glucagon-like peptide-1 (GLP-1), which controls the secretion of insulin in a glucose-dependent manner. Truncation studies on its sequence revealed the importance of the histidine residue at position 7 for receptor recognition, function, and the peptide’s insulinotropic activity. As native GLP-1 is rapidly degraded, the modified analogues Liraglutide and Semaglutide – also bearing this histidine residue – represent essential treatments for type 2 diabetes.

Sequence of the glucagon-like peptide-1 (7-37) amide:

H-His-Ala-Glu-Gly-Thr-Phe-Thr-Ser-Asp-Val-Ser-Ser-Tyr-Leu-Glu-Gly-Gln-Ala-Ala-Lys-Glu-Phe-Ile-Ala-Trp-Leu-Val-Lys-Gly-Arg-Gly-NH2

Iris Biotech offers a selection of deamino- and decarboxy-histidine derivatives, which can be used as tools for the preparation of libraries to investigate structure activity relationships leading to the generation of drugs with improved pharmacokinetics. As especially histidines are prone to racemization during peptide synthesis, the installation of deamino- or decarboxy-His at the C- or N-terminus of a peptide brings another crucial advantage as it allows to circumvent this issue due to the lack of chirality. Thus, this measure reduces the amount of undesired side-products, which might be difficult to remove.

For deamino-histidines, Iris Biotech provides the trityl protected imidazole propionic acid HAA6170, its shorter chain imidazole-4-acetic acid HAA9175 and the demethylated derivative thereof (HAA9180). HAA9175 is reported as building block for the synthesis of imidazolyl-polyethyleneimine modified nanoparticles benefiting from increased transfection efficiency as well as for the synthesis of ribonuclease mimics. Furthermore, imidazole-4-acetic acid is suggested as antagonist of GABAC receptors and partial GABAAR agonist being capable of penetrating the blood-brain barrier in vivo.


Decarboxy-histidine HAA9185 represents a trityl protected histamine and is reported as component of potent agonists of the histamine H2 and H4 receptor. It can be placed at the C-terminus of a peptide replacing natural histidine and is reported within the synthesis of truncated GLP-1 based peptides to analyze metabolic stability and pharmacokinetic properties. Other reports highlight HAA9185 as building block for potent inhibitors of farnesyltransferase and geranylgeranyltransferase-I. Its longer chain derivative HAA9190 is highlighted as fragment of selective H2R and H4R agonists and for its inhibitory activity towards the H3 receptor and the histamine N-methyltransferase.

References:

  • Histidine: A Systematic Review on Metabolism and Physiological Effects in Human and Different Animal Species; J. Moro, D. Tomé, P. Schmidely, T.-C. Demersay, and D. Azzout-Marniche; Nutrients 2020; 12: 1414. https://doi.org/10.3390/nu12051414. +
  • Structural and Kinetic Characterization of Active-Site Histidine as a Proton Shuttle in Catalysis by Human Carbonic Anhydrase II; Z. Fisher, J. A. Hernandez Prada, C. Tu, D. Duda, C. Yoshioka, H. An, L. Govindasamy, D. N. Silverman, R. McKenna; Biochemistry 2005; 44: 1097-1105. https://doi.org/10.1021/bi0480279.
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  • Acylguanidines as bioisosteres of guanidines: NG-acylated imidazolylpropylguanidines, a new class of histamine H2 receptor agonists; P. Ghorai, A. Kraus, M. Keller, C. Gotte, P. Igel, E. Schneider, D. Schnell, G. Bernhardt, S. Dove, M. Zabel, S. Elz, R. Seifert and A. Buschauer; Journal of medicinal chemistry 2008; 51: 7193-204. https://doi.org/10.1021/jm800841w
  • Potent inhibitors of farnesyltransferase and geranylgeranyltransferase-I; D. N. Nguyen, C. A. Stump, E. S. Walsh, C. Fernandes, J. P. Davide, M. Ellis-Hutchings, R. G. Robinson, T. M. Williams, R. B. Lobell, H. E. Huber and C. A. Buser; Bioorg Med Chem Lett 2002; 12: 1269-73. https://doi.org/10.1016/s0960-894x(02)00154-3
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