2007
DOI: 10.1074/jbc.m702089200
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Modulation of Serpin Reaction through Stabilization of Transient Intermediate by Ligands Bound to α-Helix F

Abstract: Mechanism-based inhibition of proteinases by serpins involves enzyme acylation and fast insertion of the reactive center loop (RCL) into the central ␤-sheet of the serpin, resulting in mechanical inactivation of the proteinase. We examined the effects of ligands specific to ␣-helix F (␣HF) of plasminogen activator inhibitor-1 (PAI-1) on the stoichiometry of inhibition (SI) and limiting rate constant (k lim ) of RCL insertion for reactions with ␤-trypsin, tissue-type plasminogen activator (tPA), and urokinase. … Show more

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Cited by 16 publications
(28 citation statements)
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“…However, it does not predict the exact time of fibrinolysis needed for successful IPFT, as well as whether or not this time correlates with the fibrinolytic activity at 0-80 minutes ( Figures 6A, 6C, and E7B) or with "fibrinolytic potential" (baseline fibrinolytic activity after activation of endogenous plasminogen; Figures 6B and E6A; 0 h uPA). Although the mechanism of intrapleural tPA processing could deviate from that of scuPA (18), the similarity in the effects of MA-33H1F7 and MA-8H9D4 on the "suicide" inhibition of tPA and uPA by PAI-1 (20)(21)(22) support testing a similar approach to enhance tPA-based IPFT. The availability of a number of anti-PAI-1 mAbs, antigen-binding fragments, and single-chain variable fragments, with stoichiometries of inhibition ranging from 1.5-2.0 to greater than 100 allows interventional flexibility, which could expedite future clinical trials.…”
Section: Discussionmentioning
confidence: 93%
See 2 more Smart Citations
“…However, it does not predict the exact time of fibrinolysis needed for successful IPFT, as well as whether or not this time correlates with the fibrinolytic activity at 0-80 minutes ( Figures 6A, 6C, and E7B) or with "fibrinolytic potential" (baseline fibrinolytic activity after activation of endogenous plasminogen; Figures 6B and E6A; 0 h uPA). Although the mechanism of intrapleural tPA processing could deviate from that of scuPA (18), the similarity in the effects of MA-33H1F7 and MA-8H9D4 on the "suicide" inhibition of tPA and uPA by PAI-1 (20)(21)(22) support testing a similar approach to enhance tPA-based IPFT. The availability of a number of anti-PAI-1 mAbs, antigen-binding fragments, and single-chain variable fragments, with stoichiometries of inhibition ranging from 1.5-2.0 to greater than 100 allows interventional flexibility, which could expedite future clinical trials.…”
Section: Discussionmentioning
confidence: 93%
“…MA-33H1F7 and MA-8H9D4 additively redirect more than 95% of the reaction of human PAI-1 with uPA or tPA to the substrate branch the PAI-1 mechanism (20). Moreover, vitronectin, which binds PAI-1 with nanomolar affinity, potentiates PAI-1 neutralization by mAbs (21)(22)(23). In this study, MA-33H1F7 and MA-8H9D4 were selected after in vitro and ex vivo testing against rabbit PAI-1, and used as Protection of urokinase (uPA) (E) from inactivation by endogenous plasminogen activator inhibitor (PAI)-1 (I) by monoclonal antibody (mAb)-mediated redirection of the mechanism from the inhibitory (k i ) to the substrate (k s ) branch.…”
Section: Clinical Relevancementioning
confidence: 99%
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“…The second-order rate constants for the inhibition of PAs with human and rabbit PAI-1 were determined using stopped flow fluorimetry. SDS-PAGE was used to compare the stoichiometry of inhibition (39) for the interactions between PAs and PAI-1 from both species, as previously described (23,40). The rates of mechanism-based inhibition of both uPA ( Figure E2) and tPA (data not shown) by PAI-1 were diffusion-limited (.…”
Section: Transduction Of Primary Rpmcs With Recombinant Adenovirusesmentioning
confidence: 99%
“…The concentration of PAI-1 is markedly increased in pleural loculation (20)(21)(22). Active PAI-1 spontaneously transitions to its inactive latent form (23), which is predominant under physiological conditions. Although high concentrations of PAI-1 antigen are likewise strongly correlated with the severity of human pleural injury (18,20,21,24), the proportion of PAI-1 that remains active in pleural injury remains unclear, and its contribution to the severity of pleural injury has not, to our knowledge, been previously studied.…”
mentioning
confidence: 99%