Role of Basic Residues of the Autolysis Loop in the Catalytic Function of Factor Xa

Manithody, Chandrashekhara; Yang, Likui; Rezaie, Alireza R.

doi:10.1021/bi0255367

Cited by 60 publications

(170 citation statements)

References 42 publications

(74 reference statements)

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“…The autolysis loop of fXa contains four basic residues at positions 143, 147, 150, and 154 (Table 1) and the Ala-scanning mutagenesis of these residues has identified Arg-150 as the critical residue that specifically interacts with AT in the presence of pentasaccharide (18). The recent X-ray crystal structure determination of a catalytically inactive mutant of fXa in complex with AT in the presence of pentasaccharide supported the mutagenesis results (26).…”

Section: Discussionmentioning

confidence: 76%

“…We investigated the mechanism by which coagulation proteases differentially react with the activated conformation of AT and demonstrated that the autolysis loop of both fXa and fIXa (residues 143-154 in chymotrypsin numbering) (16) have several basic residues that specifically interact with the serpin in the presence of pentasaccharide (17)(18)(19). Thus, we hypothesized that thrombin does not react with the heparin-activated conformation of AT because the basic residues of fXa are not conserved in the autolysis loop of the protease (17).…”

Section: Introductionmentioning

confidence: 99%

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The role of autolysis loop in determining the specificity of coagulation proteases

Yang

Manithody

Rezaie

2007

Braz J Med Biol Res

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We recently demonstrated that the substitution of the autolysis loop (residues 143 to 154 in the chymotrypsin numbering system) of activated protein C (APC) with the corresponding loop of factor Xa (fXa) renders the APC mutant (APC/fX 143-154 ) susceptible to inhibition by antithrombin (AT) in the presence of pentasaccharide. Our recent results further indicated, that in addition to an improvement in the reactivity of APC/fX 143-154 with AT, both the amidolytic and antifactor Va activities of the mutant APC have also been significantly increased. Since the autolysis loop of APC is five residues longer than the autolysis loop of fXa, it could not be ascertained whether this loop in the mutant APC specifically interacts with the activated conformation of AT or if a shorter autolysis loop is responsible for a global improvement in the catalytic activity of the mutant protease. To answer this question, we prepared another APC mutant in which the autolysis loop of the protease was replaced with the corresponding loop of trypsin (APC/Tryp 143-154 ). Unlike an ~500-fold improvement in the reactivity of APC/fX [143][144][145][146][147][148][149][150][151][152][153][154] with AT in the presence of pentasaccharide, the reactivity of APC/Tryp 143-154 with the serpin was improved ~10-fold. These results suggest that both the length and structure of residues of the autolysis loop are critical for the specificity of the coagulation protease interaction with AT. Further factor Va inactivation studies with the APC mutants revealed a similar role for the autolysis loop of APC in the interaction with its natural substrate. Correspondence

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Section: Discussionmentioning

confidence: 76%

Section: Introductionmentioning

confidence: 99%

The role of autolysis loop in determining the specificity of coagulation proteases

Yang

Manithody

Rezaie

2007

Braz J Med Biol Res

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“…Molecular modeling suggests that electrostatic fields drive, in part, the interaction of FXa with TFPI (8,9). Basic groups of TFPI would secure contacts within the acidic loop 34 -40 of FXa, whereas an acidic patch may complement the basic autolysis loop of FXa (Arg 143 , His 145 , Lys 148 , and Arg 150 ), even though mutagenesis has failed to confirm its role (53). Compared with FXa, the k a values for E36Q/E37Q/E39Q, E36K/E37K/E39K, E74Q/E76Q/E77Q, and E74K/E76K/E77K inhibition by TFPI decreased 11-, 6-, 3-, and 3-fold, respectively (Table VII).…”

Section: Figmentioning

confidence: 99%

The Elusive Role of the Potential Factor X Cation-binding Exosite-1 in Substrate and Inhibitor Interactions

Bianchini

Pike

Bonniec

2004

Journal of Biological Chemistry

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Coagulation factor X (FX) 1 is a vitamin K-dependent zymogen activated into FXa by cleavage at a single bond (Arg 15 -Ile 16 in the chymotrypsin numbering system 2 ) hydrolyzed by either of two complexes: FVIIa bound to tissue factor (TF), which triggers coagulation after injury, or FIXa associated with FVIIIa, which amplifies thrombin production after initiation of coagulation. FXa is the only endogenous prothrombin activator, but substantial thrombin production occurs only within the prothrombinase complex, where FXa binds to FVa in the presence of calcium on an appropriate phospholipid surface. Two inhibitors control FXa activity, viz. the tissue factor pathway inhibitor (TFPI) and antithrombin.Extended binding sites (exosites) play a crucial role in virtually any substrate, cofactor, or inhibitor recognition within the coagulation cascade. Perhaps best characterized is the case of thrombin taking advantage of two exosites for extended interactions in numerous functions (1). Exosite-1 is formed by a set of basic residues comprising loops 34 -40 and 70 -80, which neighbor each other in the folded structure (2); it interacts with fibrinogen, thrombomodulin, platelet activator receptor-1, FV, FVa, heparin cofactor II, and hirudin. Exosite-2, comprising loop 91-102 and helices 165-173 and 233-245 (3), is also formed by a set of basic residues that interact with heparin, with the chondroitin sulfate of thrombomodulin, and within prothrombin with kringle-2 (4). In FVII, the region corresponding to exosite-1 of thrombin is critical for FX activation (5, 6); in FIXa, this region is also important for FX activation in the absence of FVIII and for its inhibition by antithrombin in the absence of heparin (7). In contrast to thrombin, FVIIa, FIXa, and FXa share a negatively charged patch within segment 70 -80, whereas FXa is unique in that both loops 34 -40 and 70 -80 are negatively charged. Thus, the region of FXa corresponding to exosite-1 of thrombin forms a negative cluster, raising the question as to whether it could constitute a functional exosite. FXa has a unique macromolecule substrate, but exosites may also participate in its inhibition and/or in the activation of its zymogen. In fact, a number of studies have established that exosite(s) must be critical in several FXa functions. Electrostatic interactions involving loop 34 -40 of FXa appear to play a significant role in binding to the second Kunitz domain of TFPI (8,9). FXa also appears to interact with a complementary surface on pentasaccharide-activated antithrombin (10), and the region of FXa topologically equivalent to exosite-2 of thrombin seems to be involved in the binding of heparin and FVa (11). Above all, prothrombin recognition by prothrombinase undoubtedly involves one or more exosites on .In a previous study (15), we reported that the catalytic groove of FXa is minimally selective with unconstrained peptides and that FVa has little effect, if any, on this selectivity. These two observations therefore also favor the hypothesis that FXa uses seconda...

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“…and expression of wild-type FX in an expression/purification vector system has been described previously (34). The EGF-N deletion mutant of FX, lacking the exon coding for the N-terminal EGF domain of FX (FX-desEGF-N), was prepared by PCR mutagenesis methods in the same vector system as described (34).…”

Section: Mutagenesis and Expression Of Recombinant Proteins-constructionmentioning

confidence: 99%

“…This mutant was expressed in mammalian cells and purified to homogeneity as described (34). Unlike the previous mutant lacking both the Gla and EGF-N (E2-FX) (31), this mutant contains an intact Gla domain; thus, the zymogenic and enzymatic properties of this mutant could be characterized in appropriate activation complexes on phospholipid vesicles.…”

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confidence: 99%

Role of the N-terminal Epidermal Growth Factor-like Domain of Factor X/Xa

Kittur

Manithody

Rezaie

2004

Journal of Biological Chemistry

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The functional importance of the N-terminal epidermal growth factor-like domain (EGF-N) of factor X/Xa (FX/Xa) was investigated by constructing an FX mutant in which the exon coding for EGF-N was deleted from FX cDNA. Following expression and purification to homogeneity, the mutant was characterized with respect to its ability to function as a zymogen for either the factor VIIa-tissue factor complex or the factor IXa-factor VIIIa complex and then to function as an enzyme in the prothrombinase complex to catalyze the conversion of prothrombin to thrombin. It was discovered that EGF-N is essential for the recognition and efficient activation of FX by both activators in the presence of the cofactors. On the other hand, the FXa mutant interacted with factor Va with a normal apparent dissociation constant and activated prothrombin with ϳ3-fold lower catalytic efficiency in the prothrombinase complex. Surprisingly, the mutant activated prothrombin with ϳ12-fold better catalytic efficiency than wild-type FXa in the absence of factor Va. The mutant was inactive in both prothrombin time and activated partial thromboplastin time assays; however, it exhibited a similar specific activity in a onestage FXa clotting assay. These results suggest that EGF-N of FX is required for the cofactor-dependent zymogen activation by both physiological activators, but it plays no apparent role in FXa recognition of the cofactor in the prothrombinase complex.

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Role of Basic Residues of the Autolysis Loop in the Catalytic Function of Factor Xa

Cited by 60 publications

References 42 publications

The role of autolysis loop in determining the specificity of coagulation proteases

The role of autolysis loop in determining the specificity of coagulation proteases

The Elusive Role of the Potential Factor X Cation-binding Exosite-1 in Substrate and Inhibitor Interactions

Role of the N-terminal Epidermal Growth Factor-like Domain of Factor X/Xa

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