2016
DOI: 10.1073/pnas.1609375114
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Active-site MMP-selective antibody inhibitors discovered from convex paratope synthetic libraries

Abstract: Proteases are frequent pharmacological targets, and their inhibitors are valuable drugs in multiple pathologies. The catalytic mechanism and the active-site fold, however, are largely conserved among the protease classes, making the development of the selective inhibitors exceedingly challenging. In our departure from the conventional strategies, we reviewed the structure of known camelid inhibitory antibodies, which block enzyme activities via their unusually long, convex-shaped paratopes. We synthesized the … Show more

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Cited by 75 publications
(120 citation statements)
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“…105 By contrast, sdAb paratopes can clearly adopt both flat 106,107 and convex 11 topologies, although possibly only inefficiently adopt concave ones. The CDR1 and CDR2 loops of V H Hs depart from the typical canonical structures of conventional antibodies (Figure 2A), potentially through somatic mutation since germline human V H and camelid V H H repertoires appear to have similar canonical structures.…”
Section: Single-domain Antibody Paratope Structuresmentioning
confidence: 99%
“…105 By contrast, sdAb paratopes can clearly adopt both flat 106,107 and convex 11 topologies, although possibly only inefficiently adopt concave ones. The CDR1 and CDR2 loops of V H Hs depart from the typical canonical structures of conventional antibodies (Figure 2A), potentially through somatic mutation since germline human V H and camelid V H H repertoires appear to have similar canonical structures.…”
Section: Single-domain Antibody Paratope Structuresmentioning
confidence: 99%
“…Scheme that convex antibody paratope formed by an extended CDR-H3 mediates enzyme inhibition (reprinted from Ref [24]).…”
Section: Figurementioning
confidence: 99%
“…Typical results of MMP inhibitory Fab characterizations (reprinted from Ref [24]). (A) Binding affinity and inhibition potency measured by ELISA and FRET assays.…”
Section: Figurementioning
confidence: 99%
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“…2C), which was 20-fold weaker than KD1. Notably, inhibitors that demonstrate protease binding do not always demonstrate protease inhibition of the target active site (47,48). Thus, proteins were tested for functional matriptase inhibition by incubating an increasing number of yeast cells displaying KD2/1 or wild-type KD1 or KD2 with soluble matriptase and substrate.…”
Section: Engineering the Kunitz Domain 2 (Kd2) Of Hai-1 To Bind Matrimentioning
confidence: 99%