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1 calfactant) and yet to be described effects (activated protein C).
2 slower time scale, spontaneously converts to activated protein C.
3 ike serine proteases thrombin, factor Xa, or activated protein C.
4 s anti-inflammatory properties when bound by activated protein C.
5 were independent of its ability to generate activated protein C.
6 associated with the use of recombinant human activated protein C.
7 GH patterns, and GH modulated resistance to activated protein C.
8 ty-three patients received recombinant human activated protein C.
9 agulant versus anti-inflammatory function of activated protein C.
10 inflammatory and anti-apoptotic functions of activated protein C.
11 or Va partially resistant to inactivation by activated protein C.
12 rombin, factors VIIa, Xa, XIa, and XIIa, and activated protein C.
13 tor for the thrombin-dependent generation of activated protein C.
14 ffinity and blockade activity for its ligand activated protein C.
15 heparan-sulfate-accelerated antithrombin and activated protein C.
16 al myosin provides membrane-like support for activated protein C.
17 matory activity of rTMD23 was independent of activated protein C.
18 cell could be prevented by recombinant human activated protein C.
19 phase III clinical trial was human recumbent activated protein C.
20 ween observational and randomized studies of activated protein C.
21 d in patients treated with recombinant human activated protein C.
22 hanced enzymatic activity of factor VIIa and activated protein C.
23 presence of tissue factor, thrombomodulin or activated protein C.
24 als and the recent withdrawal of recombinant activated protein C.
25 associated with the use of recombinant human activated protein C (108/311 [34.7%] vs. 254/622 [40.8%]
26 ombin-thrombomodulin-dependent generation of activated protein C, a natural anticoagulant, binds to a
28 odulin-protein C pathway are consistent with activated protein C activation and systemic anticoagulat
29 with the institution of a recombinant human activated protein C administration policy from the first
30 rodents, we now show that administration of activated protein C alone or in combination with tissue
33 TM catalyzes thrombin-mediated generation of activated protein C and binds to circulating RBCs withou
34 Ill Patients with Septic Shock) and $30,911 (Activated Protein C and Corticosteroids for Human Septic
35 ritically Ill Patients with Septic Shock and Activated Protein C and Corticosteroids for Human Septic
36 ritically Ill Patients with Septic Shock and Activated Protein C and Corticosteroids for Human Septic
38 by generating pharmacological quantities of activated protein C and effectively diagnoses protein C
39 s factor, which suppresses the generation of activated protein C and increases TF, augmented FX activ
40 able model assessing the association between activated protein C and mortality resulted in a 9% shift
42 d to endothelial cell protein C receptor) to activated protein C and this generates antiinflammatory
43 cing cofactor for the coagulation inhibitors activated protein C and tissue factor pathway inhibitor
44 older drugs, newer drugs, drotrecogin alpha (activated protein C) and activated factor VII concentrat
45 arameters, including soluble thrombomodulin, activated protein C, and disseminated intravascular coag
48 In addition to an anticoagulant activity, activated protein C (APC) also exhibits anti-inflammator
49 n of protease-activated receptor 1 (PAR1) by activated protein C (APC) and thrombin elicits paradoxic
53 nflammatory and cytoprotective properties of activated protein C (APC) are mediated through its endot
55 is revealed that FVII, FVIIa, protein C, and activated protein C (APC) bound to EPCR with similar aff
57 protein, accelerates in vitro generation of activated protein C (APC) by soluble thrombin/thrombomod
58 hrough 2 mechanisms: decreased generation of activated protein C (APC) by thrombin, and resistance to
59 antibodies are able to inhibit generation of activated protein C (aPC) by thrombin/thrombomodulin (II
60 n, which results in suppressed generation of activated protein C (APC) by TM-thrombin complex and in
61 ion of PS by purified CK1 did not affect its activated protein C (APC) cofactor activity in activated
62 xamination of the structure of Gla domain of activated Protein C (APC) complexed with soluble endothe
63 ontained in the 39-, 60-, and 70-80-loops of activated protein C (APC) comprise an exosite that contr
67 WE thrombin acts as an anticoagulant through activated protein C (APC) generation, the observed limit
87 al. report that the endogenous anticoagulant activated protein C (APC) is able to cross the blood-spi
94 Here we identify the thrombomodulin (Thbd)-activated protein C (aPC) pathway as a new mechanism for
98 sm of protease-activated receptor (PAR) 1 by activated protein C (APC) provides neuro- and vasculopro
99 ssue of Blood, Sinha et al demonstrated that activated protein C (APC) reduced the severity of pulmon
103 Endothelial barrier protective effects of activated protein C (APC) require the endothelial protei
104 n (FV Trp1920-->Arg, FVNara) associated with activated protein C (APC) resistance and a severe thromb
105 we measured factor V Leiden, HR2 haplotype, activated protein C (APC) resistance, and plasma factor
107 tion of PAR1 with the anticoagulant protease activated protein C (APC) results in activation of Ras-r
110 mmatory signaling, whereas its activation by activated protein C (APC) stimulates cytoprotective and
111 els provide a microenvironment enriched with activated protein C (aPC) that retains EPCR(+) LT-HSCs b
115 hat Zn(2+) enhanced the binding of protein C/activated protein C (APC) to endothelial cell protein C
116 hesion and compared the protective effect of activated protein C (APC) to that of the Food and Drug A
119 To discuss the potential use of recombinant activated protein C (aPC) variants with altered bioactiv
131 on newly discovered biological properties of activated protein C (APC), an endogenous plasma protease
132 wever, factor Va is prone to inactivation by activated protein C (APC), an important serine protease
134 r molecule of the natural protein C pathway, activated protein C (aPC), exerts pleiotropic effects on
135 anticoagulant human plasma serine protease, activated protein C (APC), inhibits blood coagulation by
137 ks the contact system, but also thrombin and activated protein C (APC), making it an unattractive can
138 anticoagulant and anti-inflammatory enzyme, activated protein C (APC), naturally controls thrombosis
139 hough ProS is known to act as a cofactor for activated Protein C (aPC), plasma from Pros1+/- heterozy
141 rectly precede the Arg-506 cleavage site for activated protein C (APC), the 499-505(VIII) FVa mutant
144 eceptor, accelerates the conversion of PC to activated protein C (APC), which leads to the down-regul
145 ity toward cleavage of plasma protein C into activated protein C (APC), which opposes its thrombotic
146 s discovered to play a key role in mediating activated protein C (APC)-induced cytoprotective effects
147 The effect of glucosylceramide (GlcCer) on activated protein C (APC)-phospholipid interactions was
154 several serine proteases (such as thrombin, activated protein C [APC], and plasmin) involved in hemo
155 leaved by the anticoagulant serine protease, activated protein C, at two cleavage sites, Arg(336) in
157 ia isolates was sufficient to interfere with activated protein C-barrier protective activities in hum
158 , in patients who received recombinant human activated protein C before 24 hrs there was a reduction
160 Overall, our results show that FVIIa or activated protein C binding to EPCR promotes EPCR endocy
162 EPCR), a cellular receptor for protein C and activated protein C, but the physiologic significance of
164 t-derived FVa was 2-3-fold more resistant to activated protein C-catalyzed inactivation than purified
165 factor VIIIa, we engineered mutations of the activated protein C cleavage sites into the disulfide bo
166 To isolate the effects of the individual activated protein C cleavage sites on factor VIIIa, we e
170 ed protein C, it functions as a cofactor for activated protein C-dependent proteolytic inactivation o
171 oviding the surface for thrombin generation, activated protein C did increase the time until the burs
173 lar treatment benefit from recombinant human activated protein C (drotrecogin alfa [activated]) as no
176 endotoxin trial evaluating recombinant human activated protein C (drotrecogin alfa [activated]).
177 ndomized controlled trial, recombinant human activated protein C (drotrecogin alfa) reduced mortality
178 and mortality resulted in a 9% shift in the activated protein C effect estimate toward the null (odd
179 generates antiinflammatory signals along the activated protein C-endothelial cell protein C receptor-
180 cogin alfa (activated) (or recombinant human activated protein C) excluded patients with specific bas
181 ) or at the level of factor V proteolysis by activated protein C (factor V Leiden mice), were employe
183 eatment, low VT ventilation for ALI/ARDS and activated protein C for severe sepsis (the leading cause
184 e FVL mutation accelerates thrombin and APC (activated protein C) formation in carriers without a his
186 s, the group that received recombinant human activated protein C had a significantly reduced associat
197 id and vasopressor therapy (2C); recombinant activated protein C in patients with severe sepsis and c
199 the efficacy and safety of human recombinant activated protein C in severe sepsis is limited, especia
202 recent investigations have attributed novel activated protein C-independent functions of protein S t
203 n proteases, such as fXa (factor Xa) or aPC (activated protein C), independently modulate intracellul
204 ms "activated protein C," "recombinant human activated protein C," "inflammation," "leukocyte adhesio
206 effector protease of the protein C pathway, activated protein C, interacts with the endothelial cell
209 luated phase II and III trials assuming that activated protein C is truly effective; they showed that
211 s anticoagulant activity; in the presence of activated protein C, it functions as a cofactor for acti
213 ction and/or endocytosis, viz., receptor for activated protein C kinase 1 (RACK1), muscle integrin bi
214 omplex starch solutions to recombinant human activated protein C, large multicenter randomized contro
215 investigate the effect of sustained elevated activated protein C levels on the host response during m
216 ated with protein C had significantly higher activated protein C levels than children receiving place
217 aPL+) compared to healthy controls, but anti-activated protein C levels were not increased in these p
220 ting with septic shock, early treatment with activated protein C may be associated with reduced hospi
225 across the spectrum of ineffective therapy (activated protein C), novel therapeutic ideas (statins a
227 y contrast, whenever platelets were present, activated protein C only minimally affected the amount o
229 reports on the efficacy of recombinant human activated protein C, or drotrecogin alfa (activated) (Dr
230 neutralizing agents such as antihistone IgG, activated protein C, or heparin prevented this effect.
232 al administration rates of recombinant human activated protein C over the same timeline (p<.001), wit
234 Plasma activated protein C concentrations in activated protein C overexpressing mice (median 18.1 ng/
238 urthermore, activation of the thrombomodulin-activated protein C pathway in the regions between sites
240 Similarly, there is preferential binding of activated protein C (PC) to Gr1(high)CD11b(high)VLA-3(hi
241 uences were tested for binding to protein C, activated protein C, plasmin, factor VIIa (FVIIa), FIX,
242 ate that the natural anticoagulant protease, activated protein C, potently inhibits polyP-mediated pr
244 tural anticoagulants (low antithrombin, high activated protein C, protein S, and tissue factor pathwa
245 tithrombin complex, antithrombin, protein C, activated protein C, protein S, soluble endothelial prot
246 On univariable analysis, fibrinogen, low activated protein C ratio, D-dimer, tissue plasminogen a
247 th administration rates of recombinant human activated protein C reaching 9.2% in the last quarter.
248 tro data and a MEDLINE search for the terms "activated protein C," "recombinant human activated prote
249 ivo administration of hirudin or recombinant activated protein C reduced disease severity in experime
250 Recently, treatment with recombinant human activated protein C reduced mortality 6% compared with c
253 dermal hormone-replacement therapy increases activated protein C resistance independently of the pres
254 authors suggest that functional testing for activated protein C resistance is cheaper and more clini
260 g for thrombomodulin-dependent generation of activated protein C's (APC) anticoagulant, anti-inflamma
261 ctivation efficiency, and down-regulation by activated protein C showed similar results for the two v
262 dministration of mutant forms of recombinant activated protein C showed that both its anticoagulant a
264 have shown improved outcome with the use of activated protein C, steroid replacement and aggressive
265 her putative mechanisms of recombinant human activated protein C, such as inhibition of apoptosis and
267 trials, for example, studies of recombinant activated protein C, talactoferrin, interleukin-1 recept
268 ere more likely to receive recombinant human activated protein C than patients in South America (4.2%
269 re of two of these proteins, factor VIIa and activated protein C, than did equivalent bilayers contai
270 those who did not receive recombinant human activated protein C, the reduction in the adjusted hospi
271 esuscitate status on the association between activated protein C therapy and mortality, an associatio
273 receptor (EPCR) is crucial for signaling by activated protein C through PAR1, but EPCR may have addi
274 hrombin, factor X, activated factor VII, and activated protein C to seven different binary lipid comp
275 the patients who received recombinant human activated protein C to those who did not receive recombi
277 with a component of the coagulation system (activated protein C) to treat patients with severe sepsi
278 gher proteolytic activity by factor VIIa and activated protein C toward their natural substrates (fac
280 Compared to the entire cohort, the 1576 activated protein C-treated patients included in the mat
282 goals; corticosteroids and human recombinant activated protein C use) (all I2 > or = 67%, p < .002).
284 all covariates achieved balance, receipt of activated protein C was associated with reduced hospital
285 septic shock, early use of recombinant human activated protein C was associated with reduced mortalit
291 rombin and the anticoagulant serine protease-activated protein C were replaced with the corresponding
292 cenarios based on three published studies on activated protein C were used as real examples for stati
293 novel treatments, such as recombinant human activated protein C, which improves survival in patients
294 e micelle corona for the local generation of activated protein C, which inhibits the formation of thr
295 ical and structural analyses on thrombin and activated protein C, which suggested that residue 192 ma
296 severe sepsis who received recombinant human activated protein C with baseline bleeding precautions a
298 n 2001 on the basis of the Recombinant Human Activated Protein C Worldwide Evaluation in Severe Sepsi
299 placebo-controlled trial (human recombinant activated Protein C Worldwide Evaluation of Severe Sepsi
300 ing for how much bias in favor of or against activated protein C would be observed in single-arm stud