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HEMOSTASIS, THROMBOSIS, AND VASCULAR BIOLOGY
From the First Department of Internal Medicine,
Department of Biochemistry, and Institute for Laboratory Animal
Research, Nagoya University School of Medicine, and the Department of
Medical Technology, Nagoya University School of Health Sciences, Nagoya
National Hospital, Japan.
Antithrombin (AT) deficiency is an autosomal disorder associated
with venous thromboembolism. However, a diagnosis of homozygous AT
deficiency is seldom made. Most patients are heterozygous and have
approximately 50% AT activities, and they are at higher risk for the
development of thromboembolism. Through gene targeting we generated
AT-deficient mice and previously reported that completely AT-deficient
mice could not survive the prenatal period because of extensive
thrombosis in the myocardium and liver sinusoids. In contrast,
heterozygous AT-deficient mice with 50% AT activities have not shown
spontaneous thromboembolic episodes. To demonstrate a thrombotic
tendency in heterozygous AT deficiency, we challenged heterozygous
AT-deficient mice (AT+/ Antithrombin (AT) is a plasma glycoprotein
with a molecular weight of 58 000. It is one of the most important
inhibitors of blood coagulation, and it inactivates thrombin and
several serine proteases, including factors IXa, Xa, Xia, and XIIa, by
forming a 1:1 molar complex between the active site of the serine
protease and its reactive site. Heparin has an accelerating effect on
the formation of AT-protease complexes. In the presence of heparin, the active site of the protease is brought into close contact with the
reactive site of AT, and the rate of inhibition is enhanced up to
several thousand times.1-4
Congenital AT deficiency is an autosomal disorder associated with
venous thromboembolism. The mean prevalence of venous thromboembolism among heterozygous subjects was 51% compared with controls
without the deficiency (1.5%).5 The
incidence of the disorder in the general population is estimated at 1 in 2000 to 5000.6,7 AT deficiency is classified into 2 types. Type 1 is a quantitative deficiency, and AT antigens and
activities are lowered. Type 2 is a qualitative defect without
reduction of AT antigens.2,8 Patients with
undetectable AT activities or antigens appear to have homozygous AT
deficiency, but homozygous AT deficiency is extremely rare. Such
patients have been reported to have severe thrombotic diseases of early
onset.9 Most patients with AT deficiency are heterozygous,
and AT activity is approximately half the normal level. Previous
population studies had indicated that heterozygous patients were
expected to live as long as the general population in spite of the
greater risk for thromboembolic episodes.10,11
We generated congenitally AT-deficient mice through gene targeting and
reported that completely AT-deficient mice could not survive the
prenatal period because of extensive thrombosis in the myocardium and
liver sinusoids along with massive bleeding.12 In
contrast, heterozygous AT-deficient mice (AT+/ Mice
Assays for antithrombin
Thrombogenic challenge Mice were injected intraperitoneally with 5 mg/kg LPS (Escherichia coli serotype 0111: B4; Sigma, St Louis, MO). Four hours later, mice were killed and the lungs, livers, hearts, and kidneys were removed and fixed overnight in Carnoy solution (methanol:chloroform:acetic acid, 6:3:1). For the rescue experiment of thrombotic disease, AT+/ mice were injected through the
tail vein with AT concentrates purified from human plasma (Welfide,
Osaka, Japan) at doses of 50 U/kg or with physiological saline 30 minutes before LPS challenge.
In another experiment, mice were exposed to restraint stress by placement in 50-mL conical centrifuge tubes in which they could hardly move (Yamamoto et al, manuscript submitted). Air and water were supplied through small punctures in the tube walls. After 20 hours, the mice were killed, and their organs were removed and used for immunohistochemical analysis. Immunohistochemical analysis Fixed tissues were dehydrated, embedded in paraffin, and sectioned (6 µm thick). Tissue sections were deparaffinized in xylene, transferred to 100% ethanol, and incubated for 30 minutes in 0.3% hydrogen peroxide-methanol. After rinsing with phosphate-buffered saline (PBS), the slides were incubated successively with 5% normal goat serum-PBS (20 minutes, room temperature), rabbit anti-human fibrin-fibrinogen antibody (DAKO, Glostrup, Denmark) (1:100 dilution, 1 hour, room temperature), anti-rabbit IgG antibody conjugated with biotin (1:500 dilution, 1 hour, room temperature), and avidin-biotin complex conjugated with horseradish peroxidase (Vector Laboratories, Burlingame, CA) (30 minutes, room temperature). Staining was visualized with diaminobenzidine tetrahydrochloride-Ni3+, Co2+ (Amersham Pharmacia Biotech, Piscataway, NJ). The percentage of the glomeruli with fibrin deposition (%GFD) was calculated in all areas of each histologic specimen of the kidney. Partially stained glomeruli were categorized as positive (Figure 2A).Statistical analysis Stat-View 4.5 (SAS Institute, Cary, NC) was used for statistical analysis. P values were calculated using the Student t test, and P = .05 was considered statistically significant. Data represented means ± SD.Genotype determination of AT+/
Genotypes and plasma AT levels of AT+/ and AT+/+ mice, and the genotypes were
determined by PCR analysis. All 141 pups grew normally; 66 pups were
AT+/, and 75 were AT+/+. There was no deviation
between the 2 genotypes, indicating that the AT+/ genotype
does not cause embryonic lethality (Figure 1A). The external appearance of
AT+/ mice could not be distinguished from that of
AT+/+ mice. No spontaneous thromboembolic episodes were
observed during the longest follow-up period of 14 months. In humans,
pregnant women are at risk for thrombotic disease, but no AT+/
female mice developed thrombosis during gestation.
Plasma levels of AT antigens and activities were determined for 8 AT+/ Lipopolysaccharide challenge of AT+/ mice that were intraperitoneally injected with 5 mg/kg LPS (Figure 2A). Fibrin
deposition was also detected in the liver sinusoids (Figure 2B) and
small vessels of the myocardium (Figure 2C). We previously found that
the AT/ fetus developed degeneration of the myocardium
and liver from extensive fibrin deposition,12 but it did
not occur in AT+/ mice. In the lung, no fibrin deposition
was observed (Figure 2D). Fibrin deposition in the kidney, liver, and
myocardium was also observed in AT+/+ mice after LPS
challenge, but their levels were lower than those of AT+/
mice (data not shown). All mice survived after LPS
administration.
To compare the degree of fibrin deposition in the kidney, we
determined the %GFD and compared it between AT+/
Restraint stress It has been reported that mental or physical stress may affect coagulation level or fibrinolytic factors.13,14 Our preliminary observations suggest that restraint stress is a risk factor for thrombosis (Yamamoto et al, manuscript submitted), and we restrained AT+/+ and AT+/ mice by placing them
in narrow centrifuge tubes for 20 hours. Figure 3B indicates that the
%GFD was significantly higher in AT+/ mice than in
AT+/+ mice (28.1% ± 11.4% vs 14.9% ± 7.1%,
n = 8, P < .05).
AT supplementation before lipopolysaccharide challenge Next we studied whether AT supplementation before LPS challenge could rescue the kidney thrombus formation in AT+/ mice. To determine the appropriate dosage to which to increase plasma AT
activities, human AT concentrates were intravenously administered to
AT+/ mice at doses of 0, 25, 50, 100, and 250 U/kg. Thirty minutes later, plasma levels of AT activities were measured, and the
mean levels were 46.7%, 73.9%, 103.6%, 152.4%, and 261.5%, respectively (n = 3). Thus we chose 50 U/kg AT concentrates to normalize plasma AT levels of AT+/ mice.
The same volume of human AT concentrates or physiological saline was
injected into the tail veins of AT+/
During our 14-month observation period, no heterozygous AT-deficient mice developed spontaneous thrombotic disease. In patients with heterozygous AT deficiency, decreased plasma AT levels may not be the absolute risk factor for thrombosis but may play an additional and important role with other risk factors.3,15 In most instances, thromboembolic episodes of such patients are associated with acquired conditions, including acute infection, surgery, pregnancy, delivery, major trauma, and the use of oral contraceptives.15 Other genetic risk factors such as factor V Leiden also predispose to the development of thrombosis in heterozygous AT-deficient subjects.16 LPS or endotoxin is the specific cell membrane component of
microorganisms, and it triggers the activation of the coagulation cascade.17 We induced a hypercoagulable state in
AT+/ Systemic infectious diseases occasionally lead to the release of
endotoxin, a major thrombogenic agent. Indeed, thromboembolic episodes
of patients with heterozygous AT deficiency are reported to be
associated occasionally with acute infection,15 suggesting that patients with heterozygous AT deficiency are susceptible to
endotoxin-induced hypercoagulation. Our experiment clearly indicated
that prophylactic AT supplementation successfully rescued the
thrombotic kidney disease of AT+/ The improved %GFD achieved by AT supplementation (Figure 4) was
still higher than %GFD of AT+/+ mice (Figure 3A), which
were also challenged by LPS without pretreatment (28.5% ± 12.4% vs 19.7% ± 10.3%; P = .07). It has been reported that
plasma AT levels begin to decrease early in sepsis because of excessive
consumption.20,21 Indeed, AT activities of AT+/ Mental or physical stress appears to affect plasma coagulation
and fibrinolysis. In humans, it is one of the triggers of unstable angina, myocardial infarction, and sudden death.22-24 The
levels of several coagulation or fibrinolytic factors In this study, we confirmed that congenital heterozygous AT deficiency
is associated with a tendency to thrombosis as well as complete AT
deficiency, but these disorders are not identical in pathophysiology.
AT+/
We thank Takayuki Nakayama and Kyosuke Takeshita for their helpful advice and discussions. We greatly thank Kazuo Kagami, Kayo Sakakura, and Eriko Yamafuji for their technical assistance.
Submitted October 11, 2001; accepted November 27, 2001.
Supported in part by Grants-in-Aid for Scientific Research (11470209 and 13470203) from Ministry of Education, Science, Sports and Culture, Center of Excellence Research (COE), and Welfide Medicinal Research Foundation (H.S.).
The publication costs of this article were defrayed in part by page charge payment. Therefore, and solely to indicate this fact, this article is hereby marked "advertisement" in accordance with 18 U.S.C. section 1734.
Reprints: Hidehiko Saito, First Department of Internal Medicine, Nagoya University School of Medicine, 65 Tsurumai-cho, Showa-ku, Nagoya, Aichi 466-8550, Japan; e-mail: hsaito{at}med.nagoya-u.ac.jp.
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© 2002 by The American Society of Hematology.
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  T. Fukuda, Y. Honda, C. Matsumoto, N. Sugiyama, T. Matsushita, M. Yanada, Y. Morishima, and T. Shibano Impact of Antithrombin Deficiency on Efficacies of DU-176b, a Novel Orally Active Direct Factor Xa Inhibitor, and Antithrombin Dependent Anticoagulants, Fondaparinux and Heparin. Blood (ASH Annual Meeting Abstracts), November 16, 2005; 106(11): 1874 - 1874. [Abstract]
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 G. Schabbauer, M. Tencati, B. Pedersen, R. Pawlinski, and N. Mackman PI3K-Akt Pathway Suppresses Coagulation and Inflammation in Endotoxemic Mice Arterioscler. Thromb. Vasc. Biol., October 1, 2004; 24(10): 1963 - 1969. [Abstract] [Full Text] [PDF]
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M. Levi, J. Dorffler-Melly, P. Reitsma, H. Buller, S. Florquin, T. van der Poll, and P. Carmeliet Aggravation of endotoxin-induced disseminated intravascular coagulation and cytokine activation in heterozygous protein-C-deficient mice Blood, June 15, 2003; 101(12): 4823 - 4827. [Abstract] [Full Text] [PDF]
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K. Yamamoto, T. Shimokawa, H. Yi, K.-i. Isobe, T. Kojima, D. J. Loskutoff, and H. Saito Aging and obesity augment the stress-induced expression of tissue factor gene in the mouse Blood, December 1, 2002; 100(12): 4011 - 4018. [Abstract] [Full Text] [PDF]
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| Copyright © 2002 by American Society of Hematology Online ISSN: 1528-0020 | |||||||||
Top
Abstract
Introduction
including von
Willebrand factor, factor VIII, factor VII,