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  • blood pressure  (3)
  • Fibrin degradation products  (2)
  • Fibrinspaltprodukte  (2)
  • 1
    Electronic Resource
    Electronic Resource
    Hypercoagulability in the nephrotic syndrome (1980)
    Springer
    Journal of molecular medicine 58 (1980), S. 1029-1036 
    Details
    ISSN: 1432-1440
    Keywords: Nephrotisches Syndrom ; Thrombosen ; Fibrinspaltprodukte ; Thrombozyten ; Beta-Thromboglobulin ; Plättchenfaktor 4 ; Prostaglandine ; Nephrotic syndrome ; Coagulation ; Thrombosis ; Fibrin degradation products ; Platelets ; Beta thromboglobulin ; Platelet factor 4 ; Prostaglandins
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Description / Table of Contents: Summary The risk of thromboembolic complications in patients with the nephrotic syndrome (NS) is higher than in any other condition encountered in internal medicine. Such thromboembolic complications comprise venous thromboses (calf, thigh, renal vein) with or without pulmonary embolism and arterial thromboses (coronary thromboses, cerebral artery thromboses, peripheral arterial thromboses). Several defects of the plasmatic coagulation system, fibrinolysis and platelet function had been recognized in the nephrotic syndrome. Increased hepatic synthesis causes a rise of coagulation factors, I, II, VII, VIII, X and increased renal loss causes lowering of the plasma concentration of antithrombin III concentration. There is little evidence for DIC. Plasminogen concentration is diminished, whereas total antiplasmin activity is increased. Low alpha-1-antitrypsin concentration secondary to renal loss is outweighed by increased concentrations of other inhibitors especially alpha-2-macroglobulin and alpha-2-antiplasmin. The common presence of material in the urine reacting as fibrin degradation products with passive hemagglutination techniques appears to be proteolytically degraded fibrinogen excreted as a result of non-selective glomerular proteinuria. Platelet counts are normal or slightly elevated and platelet survival time is slightly, decreased. Definite abnormalities of spontaneous aggregation and ADP- or collagen-induced aggregation are demonstrable. Furthermore, arachidonic acid induced platelet aggregation and malondialdehyde formation by platelets of NS patients are increased. Addition of albumin to platelets of NS patients normalises platelet aggregation. This finding points to some acquired defect of platelet function. There is a clearcut relation between the risk of thromboembolic complications and plasma albumin concentration: thromboses are particularly frequent at plasma albumin concentrations below 2 g/dl. Consequently, it is suggested, that NS patients with plasma albumin 〈2 g/dl should be given platelet aggregation inhibitors prophylactically. If there is a history of venous thrombosis, long term anticoagulation with dicumarol is indicated.
    Notes: Zusammenfassung Das nephrotische Syndrom (NS) ist die intern-medizinische Grunderkrankung mit dem höchsten Risiko an venösen (Unterschenkelvenen-Thrombose, Beckenvenen-Thrombose, Cava- und Nierenvenen-Thrombose ggf. mit Lungenembolie) und arteriellen (Herzinfarkt, Cerebralarterien-Thrombose, periphere arterielle Thrombose) thromboembolischen Komplikationen. Aufgrund neuerer hämostaseologischer Untersuchungen können beim NS Defekte des plasmatischen Gerinnungssystems, der Fibrinolyse und der Plättchenfunktion festgestellt werden. Infolge der globalen Synthesesteigerung hepatischer Exportproteine ist die Plasmakonzentration der meisten Gerinnungsfaktoren (speziell Faktor I, II, VII, VIII und X) gesteigert; infolge erhöhten renalen Verlustes ist die Plasma-Konzentration des Inhibitors Antithrombin III vermindert. Die Änderung der Plasma-Konzentration ist das Ergebnis gesteigerter hepatischer Synthese und/oder renalen Verlustes im Rahmen der Proteinurie. Hinweise für eine intravasale Gerinnung fanden sich — im Gegensatz zu Angaben der Literatur — in eigenen Untersuchungen nur selten. Die Plasminogenkonzentration ist vermindert, während die Gesamt-Aktivität der Plasmin-Inhibitoren erhöht ist. Allerdings ist die Alpha-1-Antitrypsin-Konzentration wegen gesteigerten renalen Verlustes meist vermindert, was jedoch durch erhöhte Konzentration anderer Inhibitioren, speziell Alpha-2-Makroglobulin und Alpha-2-Antiplasmin kompensiert wird. Obwohl im Urin Material gefunden wird, welches in der passiven Hämagglutination wie Fibrinspaltprodukte reagiert, zeigten neuere Untersuchungen, daß dieses Material Fibrinogensplatprodukte darstellt (nicht selektive glomeruläre Proteinurie) und nicht Fibrinspaltprodukte infolge lokaler oder systemischer Fibrinolyse. Die Plättchenzahlen sind normal oder mäßig erhöht und die Plättchen-Überlebenszeit ist geringfügig verkürzt. Hingegen lassen sich deutliche Abweichungen der Spontanaggregation sowie der ADP- und Kollagen-induzierten Aggregation nachweisen. Desgleichen ist die Plättchen-Aggregation durch Arachidonsäure gesteigert und die Malondialdehyd-Bildung erhöht. Die Plättchen nephrotischer Patienten weisen nach Zugabe von Albumin ein normales Aggregationsverhalten auf, was auf eine erworbene Funktionsstörung hinweist. Das wichtige Gebiet der Plättchenfunktion bei NS ist derzeit noch wenig erforscht. Aus den klinischen und hämostaseologischen Befunden wird die Forderung abgeleitet, bei Patienten mit nephrotischem Syndrom in jedem Falle Plättchen-Aggregationshemmer zu verabfolgen; bei Vorliegen venöser Thrombosen ist eine Langzeit-Antikoagulation mit Marcumar anzuraten.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF01476873
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  • 2
    Electronic Resource
    Electronic Resource
    Increased prevalence of salt sensitivity of blood pressure in IDDM with and without microalbuminuria (1995)
    Springer
    Diabetologia 38 (1995), S. 1443-1448 
    Details
    ISSN: 1432-0428
    Keywords: Insulin-dependent diabetes mellitus ; blood pressure ; salt sensitivity ; plasma renin activity ; atrial natriuretic factor ; circadian blood pressure profile
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Summary In insulin-dependent diabetes mellitus (IDDM) elevated exchangeable sodium (Na) levels are found even in the absence of hypertension, but it is not known whether this is associated with increased sensitivity of blood pressure to sodium level. To clarify this issue we compared 30 patients with IDDM (19 without and 11 with microalbuminuria, i.e. more than 30 mg albumin/day) and 30 control subjects matched for age, gender and body mass index. The subjects were studied on the 4th day of a low-salt diet (20 mmol/day) under in-patient conditions and were subsequently changed to the same diet with a high-salt supplement, yielding a total daily intake of 220 mmol Na/day. Circadian blood pressure, plasma renin activity (PRA), plasma atrial natriuretic factor (p-ANF), plasma cyclic guanosine 5′-phosphate (p-cGMP) and urinary albumin were measured. The proportion of salt-sensitive subjects, i.e. showing increment of mean arterial pressure ≥ 3 mmHg on high-salt diet, was 43% in diabetic patients (50% of diabetic patients with and 37% without microalbuminuria) and 17% in control subjects (p〈0.05). Lying and standing PRA levels on low- or high-salt diet were significantly lower in diabetic patients than in control subjects. Salt-sensitive diabetic patients had significantly higher lying ANF on high-salt (38.7±4.2 pmol/l vs 20.1±2.3 pmol/l, p〈0.005) than on low-salt diet. The results suggest that (i) the prevalence of sodium sensitivity is high in IDDM (ii) sodium sensitivity is found even in the absence of nephropathy as indicated by albuminuria.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00400605
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  • 3
    Electronic Resource
    Electronic Resource
    Blood pressure and metabolic control as risk factors for nephropathy in Type 1 (insulin-dependent) diabetes (1985)
    Springer
    Diabetologia 28 (1985), S. 6-11 
    Details
    ISSN: 1432-0428
    Keywords: Type 1 diabetes ; diabetic nephropathy ; blood pressure ; metabolic control
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Notes: Summary The respective rôles of arterial blood pressure and metabolic control in different stages of diabetic nephropathy were analyzed retrospectively in 52 sequentially-followed Type 1 (insulin-dependent) diabetic patients. A negative correlation was found between median post-prandial blood glucose and median duration of diabetes until onset of persistent proteinuria (p〈0.01). Systolic blood pressure was higher in patients who subsequently developed persistent proteinuria than those who did not (140 versus 121 mmHg; p〈0.05), but duration of the interval until onset of persistent proteinuria was not related to blood pressure. After onset of persistent proteinuria, hypertensive diabetic patients developed elevated serum creatinine concentrations more frequently than normotensive diabetic patients (67% versus 14%, p〈0.05). In these patients, the delay until elevation of serum creatinine concentration was negatively correlated with blood glucose (p〈0.01). Once serum creatinine was raised, decay of renal function occurred faster in patients with persistent than intermittent hypertension (p〈0.05). No effect of metabolic control was demonstrable at this stage of nephropathy. It is concluded that metabolic control determines the early course of diabetic nephropathy, whereas blood pressure is more important in advanced stages of nephropathy.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00276992
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  • 4
    Electronic Resource
    Electronic Resource
    Effect of moxonidine on urinary electrolyte excretion and renal haemodynamics in man (1995)
    Springer
    European journal of clinical pharmacology 48 (1995), S. 203-208 
    Details
    ISSN: 1432-1041
    Keywords: Moxonidine ; Renal haemodynamics ; imidazoline receptors ; natriuresis ; blood pressure ; healthy volunteers
    Source: Springer Online Journal Archives 1860-2000
    Topics: Chemistry and Pharmacology , Medicine
    Notes: Abstract Moxonidine and related compounds have been recently introduced into antihypertensive therapy. It is thought that these drugs exert their blood pressure lowering effect through interaction with nonadrenergic receptors in the central nervous system, i.e. imidazoline receptors, although the contribution of specific interaction with α2-receptors is still under debate. Imidazoline receptors have recently been documented in the renal proximal tubule. In experimental studies, interaction of imidazolines with these receptors decreased the activity of the Na+/H+ antiporter and induced natriuresis. To quantitate the effect of the imidazoline receptor agonist moxonidine on renal sodium handling and renal haemodynamics in man, we examined ten healthy normotensive males (aged 25 ± 4 years) in a double blind placebo-controlled study using a crossover design. Subjects were studied on a standardized salt intake (50 mmol per day). On the 7th and 10th study day they were randomly allocated to receive either i.v. placebo or i.v. 0.2 mg moxonidine. Urinary electrolyte excretion, lithium clearance (as an index of proximal tubular sodium handling), glomerular filtration rate (GFR), effective renal plasma flow (ERPF), renal vascular resistance (RVR), mean arterial blood pressure (MAP), plasma renin activity (PRA) and plasma noradrenaline (NA) levels were assessed. Injection of moxonidine did not increase fractional sodium excretion or lithium clearance. Specifically, antinatriuresis was not observed after injection of moxonidine despite a significant decrease in MAP from 91 to 85 mmHg and a significant increase in PRA. MAP and PRA did not change with administration of placebo. Injection of moxonidine did not affect GFR and RVR; ERPF decreased slightly but not significantly. Acute administration of 0.2 mg i.v. moxonidine decreased blood pressure in healthy volunteers on standardized salt intake, but did not affect natriuresis, proximal tubular sodium reabsorption or glomerular filtration rate. The absence of an antinatriuretic response despite a decrease in blood pressure suggests a direct facilitation of natriuresis by moxonidine.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF00198299
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  • 5
    Electronic Resource
    Electronic Resource
    Stauffer's syndrome in renal cell carcinoma evidence for intravascular coagulation (1980)
    Springer
    Journal of molecular medicine 58 (1980), S. 91-97 
    Details
    ISSN: 1432-1440
    Keywords: Hypernephrom ; Gamma-GT ; Alkalische Phosphatase ; Isoenzyme der alkalischen Phosphatase ; Prothrombinzeit ; Thrombinkoagulasezeit ; Alkoholtest ; Fibrinmonomerkomplexe ; Fibrinspaltprodukte ; Renal cell carcinoma ; Gamma-GT ; Alkaline phosphatase and isoenzymes ; Disseminated intravascular coagulation (DIC) ; Prothrombin time ; Thrombin coagulase time ; Ethanol gelation test ; Soluble fibrin monomer complexes ; Fibrin degradation products
    Source: Springer Online Journal Archives 1860-2000
    Topics: Medicine
    Description / Table of Contents: Summary In 40 patients with non-metastasising (n=31) and metastasising (n=9) renal cell carcinoma, evidence of Stauffer's syndrome (increase in alkaline serum phosphatase and prolongation of prothrombin time) was found in 18 patients. Prolongation of prothrombin time was not due to depletion of vitamin K-dependent coagulation factors or manifest fibrinolysis, but due to the presence of circulating fibrinogen fibrinmonomer-FDP complexes. Ethanol gelation test was found to be positive in 28/40 subjects and soluble fibrin monomer complexes were increased in 38/40 patients. The resulting disturbance of fibrinogen-fibrin conversion was reflected by an increase in thrombin coagulase time and reptilase time. These findings suggests a state of latent compensated intravascular coagulation (presumably triggered within the vascular tumor). For diagnostic purposes the most sensitive indicator is thrombin coagulase time. Thrombin coagulase time normalised after tumor resection and was positive in patients with recurrent metastases. The increase in alkaline serum phosphatase was due to an increase in the hepatic isoenzyme. Such an increase was much more common than the elevation of total alkaline serum phosphatase. Regan's isoenzyme was only found in 1 subject. In parallel, gamma-GT was elevated in 24 patients. The study shows that Stauffer's syndrome occurs more frequently than commonly assumed when thrombin coagulase time, gamma-GT and the hepatic isoenzyme of alkaline serum phosphatase are determined in patients with renal cell carcinoma. DIC and low grade fibrinolysis may account for the coagulation abnormalities of the syndrome.
    Notes: Zusammenfassung Ein Stauffer-Syndrom (erhöhte alkalische Phosphatase und verlängerte Prothrombinzeit) wurde bei 18 von 40 Hypernephrom-Patienten gefunden. Es konnte gezeigt werden, daß die verlängerte Prothrombinzeit nicht auf eine Verminderung Vitamin K-abhängiger Gerinnungsfaktoren, sondern auf zirkulierende Fibrinogen-Fibrinomer-Fibrinspaltproduktkomplexe zurückzuführen ist. Der Alkoholtest nach Godal war bei 28 von 48 Patienten positiv und erhöhte Mengen an zirkulierenden Fibrinmonomeren wurden bei 38 von 40 Patienten gefunden. Eine gesteigerte Fibrinolyse ließ sich in 19 von 40 Patienten nachweisen. Die Verlängerung der Thrombinkoagulase-und Reptilasezeit wird auf die zirkulierenden Fibrinmonomer-Fibrinspaltproduktkomplexe zurückgeführt, die die gestörte Umwandlung von Fibrinogen in Fibrin verursachen. Die vorliegenden Befunde sprechen für eine latente kompensierte intravasale Verbrauchskoagulopathie, die wahrscheinlich innerhalb des gefäßreichen Tumors ausgelöst wird. Als empfindlicher Indikator für diagnostische Zwecke erwies sich die Thrombinkoagulasezeit. Die Thrombinkoagulasezeit normalisierte sich nach chirurgischer Entfernung des Tumors und wurde nach Auftreten von Metastasen wieder pathologisch. Die Erhöhung der alkalischen Phosphatase war in der Regel nur auf einen Anstieg des hepatischen Isoenzyms zurückzuführen. Zum Nachweis des Stauffer-Syndroms erwiesen sich das hepatische Isoenzym der alkalischen Phosphatase und die Gamma-GT empfindlicher als die Gesamt-alkalische Phosphatase.
    Type of Medium: Electronic Resource
    URL: http://dx.doi.org/10.1007/BF01477193
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