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Query: UMLS:C0002895 (
sickle cell disease
)
11,747
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
More than a dozen primary hematologic disorders have been associated with ischemic stroke. Inherited deficiencies of antithrombin III, protein C, and
protein S
have been linked with stroke in case reports; optimal screening requires functional as well as antigenic assays. Antiphospholipid antibodies and lupus anticoagulants are the most frequently identified acquired states associated with ischemic stroke. Polycythemia vera,
sickle cell anemia
, sickle-C disease, and essential thrombocythemia are the major disorders of formed blood elements causing stroke. Special, step-wise screening for occult prothrombotic entities in stroke patients is recommended for young persons with stroke of uncertain cause, for those with prior venous thrombosis, for those with a family history of unusual thrombosis, and for those with no other explanation for recurrent stroke. Acquired, perhaps transient, abnormalities of platelets, coagulation inhibition, and fibrinolysis may contribute importantly to brain ischemia in synergy with other mechanisms, but at present these remain ill-defined. The contribution of prothrombotic diatheses to stroke is probably underrecognized and warrants further investigation.
...
PMID:Hematologic disorders and ischemic stroke. A selective review. 186 63
To investigate the status of the protein C-
protein S
anticoagulant pathway in
sickle cell disease
, we measured protein C, total and free
protein S
, and C4b-binding protein levels in 20 subjects with
sickle cell disease
(Hb SS or SC). Mean total and free
protein S
levels were both significantly lower in subjects with
sickle cell disease
than in normal individuals, but greater reductions were observed for free S. The free
protein S
level was below the mean -2 SD for normal subjects in 12 subjects with
sickle cell disease
; the total
protein S
level was below this level in three subjects. Mean C4b-binding protein levels were normal in subjects with
sickle cell disease
, both during painful crisis and in the steady state, and no correlation was observed between the levels of C4b-binding protein and free
protein S
, suggesting that the low free
protein S
level was not caused by increased levels of C4b-binding protein. Crossed immunoelectrophoresis of plasma samples from eight subjects with
sickle cell disease
showed marked reductions in free
protein S
, with normal levels of
protein S
bound to C4b-binding protein. In contrast to the
protein S
level, mean protein C activity was normal in subjects with
sickle cell disease
, both during painful crisis and in the steady state. However, the protein C level was below the mean -2 SD for normal subjects on at least one occasion in four subjects with
sickle cell disease
.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:Protein S deficiency in sickle cell anemia. 296 24
Seventeen parameters of coagulation and fibrinolysis were measured in 33 patients with
sickle cell disease
; 30 were tested in steady state (SS) and 19 in crisis (Cr). There were 16 patients in both groups. The same parameters were measured in 16 controls of similar ethnic origin (Black controls; BC) and 20 Caucasian controls (CC), all with HbA only. Highly significant differences (P < 0.001) between Black and Caucasian control groups were noted for: fibrinogen, fibrinopeptide-A (FPA), beta-thromboglobulin (beta TG) and D-dimer. Significant differences (P < 0.03) in plasminogen activator inhibitor (PAI) and functional antithrombin III levels were also noted. Results of the sickle cell patients were therefore compared with those of the Black controls. Sickle cell patients in SS had raised v Wf compared with BC, which increased further during Cr (P = 0.001), but showed no significant increase in fibrinogen. Functional protein C was reduced in SS (P = 0.004) but with no further fall in Cr, while free
protein S
was normal in SS but reduced in Cr (P = 0.02). Total
protein S
and ATIII were normal in SS and Cr. FPA and beta TG were not significantly raised in SS or Cr compared with BC. There were, however, highly significant increases in D-dimer and thrombin-antithrombin complexes (TAT) in both SS and Cr compared with BC (P < 0.001 for SS and Cr vs BC). Thus significant activation of coagulation with consequent increase in fibrinolysis occurs during both the sickle cell crisis and in the steady state.(ABSTRACT TRUNCATED AT 250 WORDS)
...
PMID:Changes in coagulation and fibrinolysis in patients with sickle cell disease compared with healthy black controls. 760 84
Plasma levels of free
protein S
, a vitamin K-dependent anticoagulant, are decreased in persons with
sickle cell anemia
, but the etiology of the low levels is unknown. Protein S binds to phosphatidylserine-containing phospholipids in a calcium-dependent manner. Other studies have indicated that phosphatidylserine may be abnormally present on the outer surface of the membrane lipid bilayer of sickle cells and of the spectrin-depleted vesicles they shed in vivo. We studied the binding of purified, radiolabeled
protein S
to spectrin-depleted erythrocyte membrane vesicles and to density-separated fractions of sickle and normal erythrocytes. Calcium-dependent binding of
protein S
occurred with vesicles and with well-aerated dense irreversibly sickled cells, but not with well-aerated sickle discocytes or with normal erythrocytes. These data provide further evidence that phosphatidylserine is abnormally present on the outer surface of spectrin-depleted vesicles and of irreversibly sickled cells. In addition,
protein S
binding to such sickle membranes in vivo may be responsible, in part, for the decreased levels of free
protein S
in sickle cell plasma.
...
PMID:Erythrocyte membrane vesicles and irreversibly sickled cells bind protein S. 797 2
Recent studies suggest that increased activity of the coagulation system, measured with sensitive assays for activation markers, may be important in the pathogenesis of vascular occlusion in
sickle cell disease
(
SCD
). Since most of these studies were carried out in adult patients and
SCD
is an inherited disorder with severe morbidity even in childhood, we decided to determine the activity of the coagulation system in children with
SCD
. In a prospective study markers of thrombin generation as well as coagulation inhibitors were investigated in 16 homozygous
SCD
patients and 16 age-matched control children. Significantly increased plasma concentrations of the prothrombin fragment F1+2 and of thrombin-antithrombin III (TAT) complexes were found in
SCD
patients. The levels of protein C activity and total and free
protein S
were significantly reduced in
SCD
patients as compared with control values. Plasma AT III levels were not different in the two groups. We conclude that, in children with
SCD
, evidence of enhanced thrombin generation is present, which may in part be due to reduced levels of the inhibitors proteins C and S. The clinical relevance of this coagulation imbalance has to be demonstrated.
...
PMID:Enhanced thrombin generation in children with sickle cell disease. 819 93
In
sickle cell disease
(
SCD
), vaso-occlusion is a complex process involving cellular, vascular and humoral factors and possibly thrombotic events. We studied three physiological inhibitors of the coagulation system, antithrombin III (AT III), protein C (PC) and
protein S
(PS), in three groups of subjects: 27 homozygous patients observed either in crisis or in a steady state, 23 heterozygous patients and 30 healthy subjects. PS study included the measurement of total and free PS antigen, PS activity and C4bBP antigen. In heterozygous subjects the results were similar to those of controls, but in homozygous subjects abnormalities of PS and to a lesser extent PC were observed. Values of PC were extremely variable with 10 cases lower than the normal range (2 SD of the mean) and 17 others within this range. In all cases total PS antigen was slightly reduced (77 +/- 18%, M +/- SD) with a more marked decrease of free antigen (59 +/- 17%) and normal values of C4bBP. Levels of PS activity were greatly reduced and lower than those of free antigen with a mean ratio of PS activity to free antigen of 0.6. These abnormalities were associated with significantly high concentrations of fibrinogen D-dimers. PS deficiency in
SCD
may be at least partly due to adsorption of free PS to aminophospholipids abnormally expressed on sickle cells membranes, microvesicles and activated platelets, while the discrepancy between PS activity and free antigen could reflect proteolytic inactivation of PS by traces of thrombin.
...
PMID:Decreased protein S activity in sickle cell disease. 841 63
Abnormalities of coagulation and fibrinolysis were studied in a group of 28 children and young adults with homozygous
sickle cell disease
(
SCD
), either in the steady state (n = 12) or during painful crisis (n = 16). Coagulation was explored by standard clotting tests and by measurement of prothrombin complex factors, factor VIII (VIII:C) and antithrombin III (ATIII), protein C (PC) and
protein S
(PS) activities, while fibrinolytic potential was evaluated using D-dimer, tissue plasminogen activator (t-PA) and plasminogen activator inhibitor (PAI-1) assays. In
SCD
patients, thrombin time (TT) was constantly shortened, both in the steady state (ratio to control 0.83 +/- 0.08, p < 0.0001) and in crisis (0.76 +/- 0.06, p < 0.0001). Mean levels of prothrombin complex were similar in asymptomatic patients to those in controls, but were significantly decreased during sickle cell crisis (p < 0.05 for factor V and p < 0.0001 for factors II, VII and X). Factor VIII:C was significantly increased, both in the steady state (207 +/- 35%, p < 0.0001) and during crisis (208 +/- 34%, p < 0.0001). PS activity was reduced int he steady state (81 +/- 12%, p < 0.01) and further diminished in crisis (68.5 +/- 27.5%, p < 0.001), while D-dimers were significantly elevated during sickle cell crisis (1028 +/- 675 ng/ml, p < 0.001). In all
SCD
patients, baseline levels of t-PA antigen were comparable to those in controls, whereas concentrations of PAI-1 antigen were significantly increased, either in the steady state (89.7 +/- 26.3 ng/ml, p < 0.0001) or in crisis (75.0 +/- 24.8 ng/ml, p < 0.0001). These results provide evidence for the presence of circulating activated clotting factors in
SCD
and for an imbalance of the profibrinolytic and antifibrinolytic systems most likely due to increased PAI-1 levels.
...
PMID:Abnormalities of coagulation and fibrinolysis in homozygous sickle cell disease. 897 93
Stroke is a significant complication of
sickle cell anemia
in the pediatric population. The pathophysiology of stroke in
sickle cell anemia
remains unclear. Protein C and
protein S
activities were measured in children with
sickle cell anemia
and stroke, and compared to those with
sickle cell anemia
who were neurologically normal. Results showed significantly decreased levels of both protein C and
protein S
activities in children with
sickle cell anemia
who have had a stroke. This pilot study suggests that a possible coagulopathic state in children with
sickle cell anemia
may be associated with an increased risk for cerebrovascular disease. Further research in this area is indicated.
...
PMID:Protein C and protein S activity in sickle cell disease and stroke. 901 Jul 91
Vascular occlusion has a central role in the pathophysiology of
sickle cell disease
(
SCD
) and, although there is little evidence that thrombosis alone is responsible, patients with
sickle cell disease
are known to have an ill-defined but increased thrombotic risk. The most serious complication of this in childhood is stroke which occurs in 7-10% of children and a further 14% have asymptomatic cerebrovascular disease (CVD) on imaging. We have performed a comprehensive profile of coagulation inhibitors and markers of thrombin generation in 96 children (83 nontransfused [NTx] and 13 transfused [Tx]) with steady-state
SCD
and 18 healthy sibling controls. The levels of
protein S
(free and total) and heparin cofactor II were reduced in both the NTx and Tx groups compared to controls and protein C and APC resistance ratios were reduced in the NTx group only. Antithrombin levels were not different from controls. Thrombin-antithrombin complexes and prothrombin fragment F1+2 were increased in both patient groups. In the NTx subgroups with or without CVD there were no differences for any of the parameters measured except for lower haemoglobin levels and higher white cell counts in those with asymptomatic CVD. We conclude that children with
SCD
have a reduction in levels of the majority of the coagulation inhibitors and increased thrombin generation in the steady-state and these are only partially reversed by transfusion. However, these abnormalities do not appear to play a primary role in the development of cerebrovascular disease.
...
PMID:Prothrombotic changes in children with sickle cell disease: relationships to cerebrovascular disease and transfusion. 988 16
The significance, interactions, and sources of coagulation abnormalities and their relationship to clinical severity and painful episodes in
sickle cell disease
are not clear. To evaluate this, we have examined various measures of coagulation in 37 patients with
sickle cell disease
(20 patients with HbSS disease and 17 patients with HbSC disease). Measurements have included isotypes of antiphospholipid antibodies (IgG, IgM, IgA) to specific phospholipids; proteins C (activity, total antigen) and S (activity, total and free antigen); measures of coagulation activation (prothrombin fragment 1.2, thrombin-antithrombin, fibrinopeptide A, d-dimers); indicators of clinical severity; and studies obtained during steady states and painful episodes. Results in HbSS disease showed that antiphospholipid antibodies were increased, with IgG phosphatidylserine showing the highest and most frequently increased levels (37% of patients). Protein C (activity) and
protein S
(activity, total, free antigen) were decreased (P<.01), and all measures of coagulation activation were increased (P<.001). In HbSC disease, antiphospholipid antibodies were normal, protein C (activity) and
protein S
(free antigen) were decreased (P<.001), and all measures of coagulation activation were increased (P<.02). A strong correlation was observed in HbSS disease between IgG-PS and d-dimers. Moderate correlations occurred between protein C activity and thrombin-antithrombin and fibrinopeptide A, between
protein S
activity and prothrombin fragment 1.2 and d-dimers, and between protein C and
protein S
activity. In HbSC disease, moderate and fewer correlations occurred. Significant differences between HbSS disease and HbSC disease were observed in aPLs, proteins C and S, and measures of coagulation activation. Measurements during steady states and during painful episodes were not significantly different. We conclude that the antiphospholipid antibody IgG-PS may contribute to coagulation activation in HbSS disease and that IgG-PS, protein C, and
protein S
relate to each other and jointly to measures of coagulation activation. The increased level of IgG-PS in HbSS disease most likely reflects exposure of the procoagulant phosphatidylserine on the surfaces of red cell-shed vesicles and sickle red cells, which would further affect coagulation activation. The significant differences in coagulation measures between HbSS disease and HbSC disease are consistent with differences in clinical severity between the diseases. The development of painful episodes does not appear to be related to the coagulation changes.
...
PMID:Antiphospholipid antibodies, proteins C and S, and coagulation changes in sickle cell disease. 1052 Oct 77
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