Nerve growth factor: Structure/function relationships

Bradshaw, Ralph A.; Murray‐Rust, Judith; Ibáñez, Carlos F.; McDonald, Neil Q.; Lapatto, Risto; Blundell, T.L.

doi:10.1002/pro.5560031102

Cited by 67 publications

(39 citation statements)

References 86 publications

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“…Many efforts have been devoted to design mimetics using NGF fragments. Crystallographic and molecular modeling studies of NGF/TrkA complexes (McDonald et al, 1991;McDonald and Chao, 1995;Urfer et al, 1998;Wiesmann et al, 1999), mutagenesis analysis (Ibànez et al, 1992;Kahle et al, 1992;Drinkwater et al, 1993;Shih et al, 1994;Woo et al, 1995;Krüttgen et al, 1997;Kullander et al, 1997;Rydén and Ibàñez, 1997), and chemical modification of specific amino acids (Bradshaw et al, 1994;McDonald and Chao, 1995) have indicated the hydrophilic loops 1 and 4 and the N-terminal region of NGF as the most relevant for its biological activity. Among various peptides reported in the literature, linear peptides showed inhibitory, but no agonist activity (Longo et al, 1990), and cyclic peptides corresponding to the loop 1 sequence were shown later to have a 10-fold higher inhibitory activity (LeSauteur et al, 1995).…”

Section: Introductionmentioning

confidence: 99%

A New Nerve Growth Factor-Mimetic Peptide Active on Neuropathic Pain in Rats

Colangelo¹,

Bianco²,

Vitagliano³

et al. 2008

J. Neurosci.

110

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Analysis of the structure of nerve growth factor (NGF)-tyrosine kinase receptor A (TrkA) complex, site-directed mutagenesis studies and results from chemical modification of amino acid residues have identified loop 1, loop 4, and the N-terminal region of the NGF molecule as the most relevant for its biological activity. We synthesized several peptides mimicking the two loops (1 and 4) linked together with an appropriate spacer, with or without the N-terminal region. Two peptides named NL1L4 and L1L4 demonstrated good NGF agonist activity at a concentration as low as 3 M. They induced differentiation of chick dorsal root ganglia and stimulated tyrosine phosphorylation of TrkA, but not TrkB, receptor. In addition L1L4 was able to induce differentiation of PC12 cells. More interestingly, the peptide with the highest "in vitro" activity (L1L4) was shown to reduce neuropathic behavior and restore neuronal function in a rat model of peripheral neuropathic pain, thereby suggesting a potential therapeutic role for this NGF-mimetic peptide.

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Section: Introductionmentioning

confidence: 99%

A New Nerve Growth Factor-Mimetic Peptide Active on Neuropathic Pain in Rats

Colangelo¹,

Bianco²,

Vitagliano³

et al. 2008

J. Neurosci.

110

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“…Recombinant substitution studies indicated that residues Lys 32 and Lys 34 (17) and other residues (18) are likely to interact with p75 receptors. The NGF sites interacting with TrkA have also been derived via chemical modification (11,19,20), recombinant protein (18, 20 -23), and NGF-TrkA co-crystallization approaches (24). Taken together, these studies indicate that TrkA binding sites consist of residues in NGF loop 2 (residues 40 -49), loop 4 (residues 91-97), the N terminus (residues [1][2][3][4][5][6][7][8], and the C terminus (residues 111-115).…”

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confidence: 99%

“…Multiple techniques have been used to deduce which domains of the NGF protein interact with NGF receptors (11). A peptide mapping approach in which synthetic peptides with sequences corresponding to specific NGF regions were tested for their ability to inhibit NGF activity pointed to residues 29 -35 as a key active site (12).…”

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confidence: 99%

Nerve Growth Factor (NGF) Loop 4 Dimeric Mimetics Activate ERK and AKT and Promote NGF-like Neurotrophic Effects

Xie

Tisi

Yeo

et al. 2000

Journal of Biological Chemistry

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Previous work indicating that nerve growth factor (NGF) protein loops 2 and 4 interact with TrkA receptors raise the possibility that small molecule mimetics corresponding to TrkA-interacting domains that have NGF agonist activity can be developed. We applied our previously developed strategy of dimeric peptidomimetics to address the hypothesis that loop 4 small molecule dimeric mimetics would activate TrkA-related signal transduction and mimic NGF neurotrophic effects in a structure-specific manner. A loop 4 cyclized peptide dimer demonstrated NGF-like neurotrophic activity, whereas peptides with scrambled sequence, added or substituted residues, or cyclized in monomeric form were inactive. Activity was blocked by the TrkA inhibitors K252a and AG879 but not by NGF p75 receptor blocking antibody. Dimeric, but not monomeric, peptides partially blocked NGF activity. This profile was consistent with that of a NGF partial agonist. ERK and AKT phosphorylation was stimulated only by biologically active peptides and was blocked by K252a. The ERK inhibitor U0126 blocked the neurite-but not the survival-promoting activity of both NGF and active peptide. These studies support the proof of concept that small molecule NGF loop 4 mimetics can activate NGF signaling pathways and can mimic death-preventing and neurite-promoting effects of NGF. This finding will guide the rational design of NGF single-domain mimetics and contribute to elucidating NGF signal transduction mechanisms.Nerve growth factor (NGF) 1 acts via TrkA and p75 receptors to regulate neuronal survival, promote neurite outgrowth, and up-regulate certain neuronal functions such as mediation of pain and inflammation (1-5). These actions suggest that NGF agonists or antagonists might be useful in regulating these processes (6 -8). Factors limiting therapeutic applications of the NGF protein include restricted penetration of the central nervous system and the poor medicinal properties characteristic of most proteins (9, 10). The development of small molecule mimetics with favorable chemical properties that function as agonists or antagonists that mimic or inhibit NGF functions in the appropriate biological context will be critical in advancing potential in vivo applications of NGF. Moreover, in settings in which NGF might contribute to neuronal death, pain, or inflammatory mechanisms, NGF antagonists may be particularly relevant. Creation of single domain NGF mimetics will also constitute a powerful approach for linking specific NGF domains with specific patterns of intracellular signal transduction.A NGF mimetic (agonist or antagonist) would be expected to contain structural determinants of one or more NGF active sites that interact with NGF receptors. Multiple techniques have been used to deduce which domains of the NGF protein interact with NGF receptors (11). A peptide mapping approach in which synthetic peptides with sequences corresponding to specific NGF regions were tested for their ability to inhibit NGF activity pointed to residues 29 -35 as a key active ...

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“…A first approach used chemical modification of NGF where residues receptive for different agents could be blocked and the effect analyzed (for review, see Ref. 19). Enzymatic cleavage of NGF has identified the NH 2 terminus to be critical for binding to TrkA (20 -22).…”

mentioning

confidence: 99%

Two Restricted Sites on the Surface of the Nerve Growth Factor Molecule Independently Determine Specific TrkA Receptor Binding and Activation

Kullander

Kaplan

Ebendal

1997

Journal of Biological Chemistry

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Nerve growth factor (NGF) and neurotrophin-3 (NT-3) mediate activities such as survival, differentiation, and proliferation in various subsets of neurons. In this report, we define precisely the residues in human NGF responsible for NGF biological activity and binding specificity to the neurotrophin receptor TrkA. In earlier studies we defined five amino acid residues of NGF which confer NGF-like activity to NT-3 when replacing corresponding residues in the 120-amino acid long NT-3 molecule. Using this gain-of-function strategy we report the further dissection of this functional epitope. We also define another motif separated topographically in the NGF dimer and determined to be independently responsible for NGF specificity. The first of the two motifs determined to elicit NGF specificity is defined by the residues Val-48, Pro-49, and Gln-96, which are situated in the two top ␤-loops of NGF. The second motif is represented by residues Pro-5 and Phe-7 situated in the proximal part of the NH 2 terminus. Both motifs contain structurally important residues revealing a novel principle, where specificity for neurotrophin ligand-receptor interactions could be determined by variable residues modifying the conformation of the neurotrophin backbone. These findings will enhance further the possibility of mimicking NGF with low molecular weight compounds.

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Nerve growth factor: Structure/function relationships

Cited by 67 publications

References 86 publications

A New Nerve Growth Factor-Mimetic Peptide Active on Neuropathic Pain in Rats

A New Nerve Growth Factor-Mimetic Peptide Active on Neuropathic Pain in Rats

Nerve Growth Factor (NGF) Loop 4 Dimeric Mimetics Activate ERK and AKT and Promote NGF-like Neurotrophic Effects

Two Restricted Sites on the Surface of the Nerve Growth Factor Molecule Independently Determine Specific TrkA Receptor Binding and Activation

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