Bioactive N-terminal undecapeptides derived from parathyroid hormone: The role of α-helicity

A. Barazza; A. Wittelsberger; N. Fiori; E. Schievano; S. Mammi; C. Toniolo; J. M. Alexander; M. Rosenblatt; E. Peggion; M. Chorev

doi:10.1111/j.1399-3011.2005.00207.x

Bioactive N-terminal undecapeptides derived from parathyroid hormone: The role of α-helicity

A. Barazza
, A. Wittelsberger
, N. Fiori
, E. Schievano
, S. Mammi
, C. Toniolo
, J. M. Alexander
, M. Rosenblatt
, E. Peggion^*
, M. Chorev

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

24 Scopus citations

Abstract

The N-terminal 1-34 segment of parathyroid hormone (PTH) is fully active in vitro and in vivo and it can reproduce all biological responses in bone characteristic of the native intact PTH. Recent studies have demonstrated that N-terminal fragments presenting the principal activating domain such as PTH(1-11) and PTH(1-14) with helicity-enhancing substitutions yield potent analogues with PTH(1-34)-like activity. To further investigate the role of α-helicity on biological potency, we designed and synthesized by solid-phase methodology the following hPTH(1-11) analogues substituted at positions 1 and/or 3 by the sterically hindered and helix-promoting C ^α-tetrasubstituted α-amino acids α-amino isobutyric acid (Aib), 1-aminocyclopentane-1-carboxylic acid (Ac₅c) and 1-aminocyclohexane-1-carboxylic acid (Ac₆c): Ac₅c-V-AJb-E- I-Q-L-M-H-Q-R-NH₂ (I); Aib-V-Ac₅c-E-I-Q-L-M-H-Q-R-NH ₂ (II); Ac₆c-V-Aib-E-I-Q-L-M-H-Q-R-NH₂ (III); Aib-V-Ac₆c-E-I-Q-L-M-H-Q-R-NH2 (IV); Aib-V-Aib-E-I-Q-L-M-H-Q-R- NH₂ (V); S-V-Aib-E-I-Q-L-M-H-Q-R-NH₂ (VI), S-V-Ac ₅c-E-I-Q-L-M-H-Q-R-NH₂ (VII); Ac₅c-V-S-E-I-Q-L- M-H-Q-R-NH₂ (VIII); Ac₆c-V-S-E-I-Q-L-M-H-Q-R-NH ₂ (IX); Ac₅c-V-Ac₅c-E-I-Q-L-M-H-Q-R-NH ₂ (X); Ac₆c-V-Ac₆c-E-I-Q-L-M-H-Q-R-NH ₂ (XI). All analogues were biologically evaluated and conformationally characterized in 2,2,2-trifluoroethanol (TFE) solution by circular dichroism (CD). Analogues I-V, which cover the full range of biological activity observed in the present study, were further conformationally characterized in detail by nuclear magnetic resonance (NMR) and computer simulations studies. The results of ligand-stimulated cAMP accumulation experiments indicated that analogues I and II are active, analogues III, VI and VII are very weakly active and analogues IV, V, VIII-XI are inactive. The most potent analogue, I exhibits biological activity 3500-fold higher than that of the native PTH(1-11) and only 15-fold weaker than that of the native sequence hPTH(1-34). Remarkably, the two parathyroid hormone (PTH)C^α- tetrasubstituted amino. most potent analogues, I and II, and the very weakly active analogues, VI and VII, exhibit similar helix contents. These results indicate that the presence of a stable N-terminal helical sequence is an important but not sufficient condition for biological activity.

Original language	English
Pages (from-to)	23-35
Number of pages	13
Journal	Journal of Peptide Research
Volume	65
Issue number	1
DOIs	https://doi.org/10.1111/j.1399-3011.2005.00207.x
State	Published - Jan 2005
Externally published	Yes

Keywords

C-tetrasubstituted amino acids
Nuclear magnetic resonance
Parathyroid hormone (PTH)
α-helix

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10.1111/j.1399-3011.2005.00207.x

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@article{bf5d2a95ea3a49a79ea1a4cee28a055d,

title = "Bioactive N-terminal undecapeptides derived from parathyroid hormone: The role of α-helicity",

abstract = "The N-terminal 1-34 segment of parathyroid hormone (PTH) is fully active in vitro and in vivo and it can reproduce all biological responses in bone characteristic of the native intact PTH. Recent studies have demonstrated that N-terminal fragments presenting the principal activating domain such as PTH(1-11) and PTH(1-14) with helicity-enhancing substitutions yield potent analogues with PTH(1-34)-like activity. To further investigate the role of α-helicity on biological potency, we designed and synthesized by solid-phase methodology the following hPTH(1-11) analogues substituted at positions 1 and/or 3 by the sterically hindered and helix-promoting C α-tetrasubstituted α-amino acids α-amino isobutyric acid (Aib), 1-aminocyclopentane-1-carboxylic acid (Ac5c) and 1-aminocyclohexane-1-carboxylic acid (Ac6c): Ac5c-V-AJb-E- I-Q-L-M-H-Q-R-NH2 (I); Aib-V-Ac5c-E-I-Q-L-M-H-Q-R-NH 2 (II); Ac6c-V-Aib-E-I-Q-L-M-H-Q-R-NH2 (III); Aib-V-Ac6c-E-I-Q-L-M-H-Q-R-NH2 (IV); Aib-V-Aib-E-I-Q-L-M-H-Q-R- NH2 (V); S-V-Aib-E-I-Q-L-M-H-Q-R-NH2 (VI), S-V-Ac 5c-E-I-Q-L-M-H-Q-R-NH2 (VII); Ac5c-V-S-E-I-Q-L- M-H-Q-R-NH2 (VIII); Ac6c-V-S-E-I-Q-L-M-H-Q-R-NH 2 (IX); Ac5c-V-Ac5c-E-I-Q-L-M-H-Q-R-NH 2 (X); Ac6c-V-Ac6c-E-I-Q-L-M-H-Q-R-NH 2 (XI). All analogues were biologically evaluated and conformationally characterized in 2,2,2-trifluoroethanol (TFE) solution by circular dichroism (CD). Analogues I-V, which cover the full range of biological activity observed in the present study, were further conformationally characterized in detail by nuclear magnetic resonance (NMR) and computer simulations studies. The results of ligand-stimulated cAMP accumulation experiments indicated that analogues I and II are active, analogues III, VI and VII are very weakly active and analogues IV, V, VIII-XI are inactive. The most potent analogue, I exhibits biological activity 3500-fold higher than that of the native PTH(1-11) and only 15-fold weaker than that of the native sequence hPTH(1-34). Remarkably, the two parathyroid hormone (PTH)Cα- tetrasubstituted amino. most potent analogues, I and II, and the very weakly active analogues, VI and VII, exhibit similar helix contents. These results indicate that the presence of a stable N-terminal helical sequence is an important but not sufficient condition for biological activity.",

keywords = "C-tetrasubstituted amino acids, Nuclear magnetic resonance, Parathyroid hormone (PTH), α-helix",

author = "A. Barazza and A. Wittelsberger and N. Fiori and E. Schievano and S. Mammi and C. Toniolo and Alexander, \{J. M.\} and M. Rosenblatt and E. Peggion and M. Chorev",

year = "2005",

month = jan,

doi = "10.1111/j.1399-3011.2005.00207.x",

language = "אנגלית",

volume = "65",

pages = "23--35",

journal = "Journal of Peptide Research",

issn = "1397-002X",

number = "1",

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TY - JOUR

T1 - Bioactive N-terminal undecapeptides derived from parathyroid hormone

T2 - The role of α-helicity

AU - Barazza, A.

AU - Wittelsberger, A.

AU - Fiori, N.

AU - Schievano, E.

AU - Mammi, S.

AU - Toniolo, C.

AU - Alexander, J. M.

AU - Rosenblatt, M.

AU - Peggion, E.

AU - Chorev, M.

PY - 2005/1

Y1 - 2005/1

N2 - The N-terminal 1-34 segment of parathyroid hormone (PTH) is fully active in vitro and in vivo and it can reproduce all biological responses in bone characteristic of the native intact PTH. Recent studies have demonstrated that N-terminal fragments presenting the principal activating domain such as PTH(1-11) and PTH(1-14) with helicity-enhancing substitutions yield potent analogues with PTH(1-34)-like activity. To further investigate the role of α-helicity on biological potency, we designed and synthesized by solid-phase methodology the following hPTH(1-11) analogues substituted at positions 1 and/or 3 by the sterically hindered and helix-promoting C α-tetrasubstituted α-amino acids α-amino isobutyric acid (Aib), 1-aminocyclopentane-1-carboxylic acid (Ac5c) and 1-aminocyclohexane-1-carboxylic acid (Ac6c): Ac5c-V-AJb-E- I-Q-L-M-H-Q-R-NH2 (I); Aib-V-Ac5c-E-I-Q-L-M-H-Q-R-NH 2 (II); Ac6c-V-Aib-E-I-Q-L-M-H-Q-R-NH2 (III); Aib-V-Ac6c-E-I-Q-L-M-H-Q-R-NH2 (IV); Aib-V-Aib-E-I-Q-L-M-H-Q-R- NH2 (V); S-V-Aib-E-I-Q-L-M-H-Q-R-NH2 (VI), S-V-Ac 5c-E-I-Q-L-M-H-Q-R-NH2 (VII); Ac5c-V-S-E-I-Q-L- M-H-Q-R-NH2 (VIII); Ac6c-V-S-E-I-Q-L-M-H-Q-R-NH 2 (IX); Ac5c-V-Ac5c-E-I-Q-L-M-H-Q-R-NH 2 (X); Ac6c-V-Ac6c-E-I-Q-L-M-H-Q-R-NH 2 (XI). All analogues were biologically evaluated and conformationally characterized in 2,2,2-trifluoroethanol (TFE) solution by circular dichroism (CD). Analogues I-V, which cover the full range of biological activity observed in the present study, were further conformationally characterized in detail by nuclear magnetic resonance (NMR) and computer simulations studies. The results of ligand-stimulated cAMP accumulation experiments indicated that analogues I and II are active, analogues III, VI and VII are very weakly active and analogues IV, V, VIII-XI are inactive. The most potent analogue, I exhibits biological activity 3500-fold higher than that of the native PTH(1-11) and only 15-fold weaker than that of the native sequence hPTH(1-34). Remarkably, the two parathyroid hormone (PTH)Cα- tetrasubstituted amino. most potent analogues, I and II, and the very weakly active analogues, VI and VII, exhibit similar helix contents. These results indicate that the presence of a stable N-terminal helical sequence is an important but not sufficient condition for biological activity.

AB - The N-terminal 1-34 segment of parathyroid hormone (PTH) is fully active in vitro and in vivo and it can reproduce all biological responses in bone characteristic of the native intact PTH. Recent studies have demonstrated that N-terminal fragments presenting the principal activating domain such as PTH(1-11) and PTH(1-14) with helicity-enhancing substitutions yield potent analogues with PTH(1-34)-like activity. To further investigate the role of α-helicity on biological potency, we designed and synthesized by solid-phase methodology the following hPTH(1-11) analogues substituted at positions 1 and/or 3 by the sterically hindered and helix-promoting C α-tetrasubstituted α-amino acids α-amino isobutyric acid (Aib), 1-aminocyclopentane-1-carboxylic acid (Ac5c) and 1-aminocyclohexane-1-carboxylic acid (Ac6c): Ac5c-V-AJb-E- I-Q-L-M-H-Q-R-NH2 (I); Aib-V-Ac5c-E-I-Q-L-M-H-Q-R-NH 2 (II); Ac6c-V-Aib-E-I-Q-L-M-H-Q-R-NH2 (III); Aib-V-Ac6c-E-I-Q-L-M-H-Q-R-NH2 (IV); Aib-V-Aib-E-I-Q-L-M-H-Q-R- NH2 (V); S-V-Aib-E-I-Q-L-M-H-Q-R-NH2 (VI), S-V-Ac 5c-E-I-Q-L-M-H-Q-R-NH2 (VII); Ac5c-V-S-E-I-Q-L- M-H-Q-R-NH2 (VIII); Ac6c-V-S-E-I-Q-L-M-H-Q-R-NH 2 (IX); Ac5c-V-Ac5c-E-I-Q-L-M-H-Q-R-NH 2 (X); Ac6c-V-Ac6c-E-I-Q-L-M-H-Q-R-NH 2 (XI). All analogues were biologically evaluated and conformationally characterized in 2,2,2-trifluoroethanol (TFE) solution by circular dichroism (CD). Analogues I-V, which cover the full range of biological activity observed in the present study, were further conformationally characterized in detail by nuclear magnetic resonance (NMR) and computer simulations studies. The results of ligand-stimulated cAMP accumulation experiments indicated that analogues I and II are active, analogues III, VI and VII are very weakly active and analogues IV, V, VIII-XI are inactive. The most potent analogue, I exhibits biological activity 3500-fold higher than that of the native PTH(1-11) and only 15-fold weaker than that of the native sequence hPTH(1-34). Remarkably, the two parathyroid hormone (PTH)Cα- tetrasubstituted amino. most potent analogues, I and II, and the very weakly active analogues, VI and VII, exhibit similar helix contents. These results indicate that the presence of a stable N-terminal helical sequence is an important but not sufficient condition for biological activity.

KW - C-tetrasubstituted amino acids

KW - Nuclear magnetic resonance

KW - Parathyroid hormone (PTH)

KW - α-helix

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C2 - 15686531

AN - SCOPUS:20044384535

SN - 1397-002X

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JO - Journal of Peptide Research

JF - Journal of Peptide Research

IS - 1

ER -

Bioactive N-terminal undecapeptides derived from parathyroid hormone: The role of α-helicity

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