Prediction of the three‐dimensional structures of the nerve growth factor and epidermal growth factor binding proteins (kallikreins) and an hypothetical structure of the high molecular weight complex of epidermal growth factor with its binding protein

Bax, Benjamin; Ferguson, Geraldine; Blaber, Michael; Sternberg, Michael J.E.; Walls, Peter H.

doi:10.1002/pro.5560020805

Cited by 13 publications

(8 citation statements)

References 74 publications

(54 reference statements)

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“…NGF was discovered by Levi-Montalcini and coworkers more than 50 years ago, and belongs to the neurotrophin family, which plays a crucial role in development, maintenance and regeneration of neurons [29]. NGF is part of a high molecular weight peptide, 7S-NGF, which is a complex of 130-140 kDa composed of α, β and γ subunits [68][69][70][71]. In the normal state, NGF is a target-derived neurotrophic molecule and activates two types of receptors, the tropomyosin receptor kinase A (TrkA) receptor and the p75 NTR receptor which belongs to the death receptor family.…”

Section: Discussionmentioning

confidence: 99%

To investigate the role of the nervous system of bone in steroid-induced osteonecrosis in rabbits

Wang

et al. 2010

Osteoporos Int

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Section: Discussionmentioning

confidence: 99%

To investigate the role of the nervous system of bone in steroid-induced osteonecrosis in rabbits

Wang

et al. 2010

Osteoporos Int

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“…The amino terminal residues are in green, the middle segment residues are in blue, and the carboxyl terminal residues are in red. The atomic coordinates are derived from comparative molecular modeling of porcine pancreatic kallikrein (Bode et al, 1983; see also Bax et al, 1993). Positions A82-A84 are not shown due to their absence in porcine pancreatic kallikrein.…”

Section: Structural Analysesmentioning

confidence: 99%

“…The individual amino acids involved in these contacts are presently being identified by site-directed mutagenesis. A more detailed model of EGF-BP and its interactions with EGF is described in the accompanying paper (Bax et al, 1993).…”

Section: Structural Analysesmentioning

confidence: 99%

Synthetic chimeras of mouse growth factor‐associated glandular kallikreins. II. Growth factor binding properties

et al. 1993

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Six chimeric constructs of the sequentially similar growth factor-associated kallikreins -epidermal growth factor binding protein (EGF-BP) and the y-subunit of nerve growth factor (yNGF) -have been expressed, and their ability to generate complexes with epidermal growth factor (EGF) and P-NGF, analogous to the high molecular weight forms (7s NGF and HMW-EGF) found in the mouse submaxillary gland, evaluated. The chimeras are distinguished by the interchange of three regions composing the amino, middle, and carboxyl terminal regions that encompass four surface loops possibly involved in specific growth factor interactions. Native 0-NGF (along with native a-NGF) formed complexes indistinguishable from naturally occurring 7s NGF, characterized by an q P y 2 structure (where P-NGF is itself a dimer), with recombinant (r) y-NGF and with a chimera in which the amino terminal region from EGF-BP was substituted. Two other chimeras containing either the middle or carboxyl terminal regions of y-NGF showed weaker ability to form 7s complexes. Thus, all chimeras containing two segments from y-NGF retained at least some ability to form the 7s complex. rEGF-BP reacted weakly with EGF, but the chimera composed of the amino and middle segments of EGF-BP and the carboxyl terminal segment of y-NGF formed a nativelike HMW-EGF complex. None of the other chimeras appeared to bind EGF. These results identify amino acid positions within each kallikrein that participate in strong growth factor interactions and demonstrate that, outside of active site contacts, different regions of the kallikreins are involved in the binding of EGF and 6-NGF, respectively. Keywords: enzyme hybrids; epidermal growth factor; high molecular weight complex formation; mutagenesis; nerve growth factor; recombinant proteins; surface loops Epidermal growth factor binding protein and the y-subunit of nerve growth factor are mouse glandular kallikreins with the ability to stably and reversibly associate with epidermal growth factor and nerve growth factor, respectively (Varon et al

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“…Thus, the unique kinetic characteristics for EGF-BP and y-NGF have been localized in each case to a few specific amino acid residue positions. Residues associated with growth factor interactions and hypothetical models for the kallikreins and the high molecular weight EGF complex are described in the accompanying reports (Bax et al, 1993;Blaber et al, 1993).…”

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confidence: 99%

Synthetic chimeras of mouse growth factor‐associated glandular kallikreins. I. Kinetic properties

Blaber

Isackson

Burnier³

et al. 1993

Protein Science

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A series of six chimeric proteins, composed of fragments corresponding to either one or the other of the growth factor-associated mouse glandular kallikreins -epidermal growth factor binding protein (EGF-BP) and the y-subunit of nerve growth factor (7-NGF) -were expressed in Escherichia coli and isolated, and their kinetic properties were characterized. The assembly of these synthetic proteases involved the substitution of regions of the proteins containing four specific surface loops that have been postulated to influence both kinetic specificity and the formation of growth factor complexes. The substrates utilized in the kinetic characterization of these chimeric kallikreins were tripeptide nitroanilides representing carboxyl termini of both the EGF and @-NGF mature hormones, putative processing sites for these kallikreins in the precursors. Characterization of these hybrid enzymes demonstrates that K, and kc,, kinetic constants may be independently affected by the regions utilized in construction of these chimeric kallikreins. Specifically, loop 1, located in the amino terminal region (Bode, W., et al., J.Mol. Biol. 164, 1983), in y-NGF enhanced the kc,, for substrates containing threonine in the P2 position, as is the case during the processing of the carboxy terminus of the 0-NGF precursor. Also, the central regions of the kallikreins containing loop 2 and the kallikrein loop dictated the generally inverted K , and k, , kinetic constants observed between EGF-BP and y-NGF. Finally, in y-NGF the autolysis loop, found in the carboxyl terminal region, functions to lower the K, kinetic constant for a variety of substrates. The results allow previously characterized kinetic differences between EGF-BP and y-NGF to be interpreted in terms of specific regions of the proteins and identify a subset of amino acid positions responsible for these functional characteristics.

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Prediction of the three‐dimensional structures of the nerve growth factor and epidermal growth factor binding proteins (kallikreins) and an hypothetical structure of the high molecular weight complex of epidermal growth factor with its binding protein

Cited by 13 publications

References 74 publications

To investigate the role of the nervous system of bone in steroid-induced osteonecrosis in rabbits

To investigate the role of the nervous system of bone in steroid-induced osteonecrosis in rabbits

Synthetic chimeras of mouse growth factor‐associated glandular kallikreins. II. Growth factor binding properties

Synthetic chimeras of mouse growth factor‐associated glandular kallikreins. I. Kinetic properties

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