Pathy's Principles and Practice of Geriatric Medicine. Группа авторов

Pathy's Principles and Practice of Geriatric Medicine - Группа авторов


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primarily due to intracranial and subarachnoid haemorrhage, ruptured aortic aneurysm, gastrointestinal bleeding from peptic ulcers, and gastric or colonic malignancy. Bleeding due to primary disorders of haemostasis in the elderly is relatively rare. Severe congenital bleeding diatheses are usually diagnosed at a young age, with the majority of them now being treatable and carrying a normal life expectancy, while acquired disorders of haemostasis are an uncommon cause of death except as part of the syndrome of multiorgan failure. Most bleeding in the elderly is localized and the result of a specific underlying pathology, frequently malignancy. Bleeding disorders can be classified as being due to abnormalities of platelet number or function, disorders of the coagulation cascade, and disturbances of the vascular endothelium and connective tissues.

      The normal platelet count is between 150 and 400 × 109/l. There is, however, some reserve, and haemostasis is normal with a platelet count above 80 × 109/l, assuming normal platelet function. If the platelet count falls below this value, the bleeding time progressively prolongs; but spontaneous haemorrhage, in particular intracerebral haemorrhage, does not occur until the platelet count falls below 20 × 109/l. Platelet numbers can be decreased by three mechanisms: decreased production in the bone marrow, increased peripheral destruction due to consumption (DIC), or immune destruction (ITP) and splenic pooling in gross splenomegaly with hypersplenism. In addition, prescription drugs should always be considered as a possible cause in any case of thrombocytopenia.2

      Decreased platelet production

      Decreased platelet production can be due to any condition that causes infiltration and replacement or aplasia of the bone marrow, such as aplastic anaemia, leukaemia, lymphoma, and carcinoma myelodysplasia or deficiency of vitamin B12 and folate in megaloblastic anaemia.

      Increased peripheral destruction

Test Test of Causes of abnormality
APTT Intrinsic and common pathways Factor VIII, IX, XI, XII, II, V, or X deficiency, or factor inhibitor Lupus anticoagulant Heparin
PT Extrinsic and common pathways Factor VIII, II, V, or X deficiency, or factor inhibitor Liver disease Warfarin
TT Fibrinogen polymerization A or hypo or dysfibrinogenaemia (some dysfibrinogenaemias cause thrombosis, not bleeding) Heparin
Fibrinogen Fibrinogen quantity A or hypo or dysfibrinogenaemia
FDP Fibrinolysis Disseminated intravascular coagulation Venous thrombosis
Platelet count Platelet number Thrombocytopenia or thrombocytosis
Bleeding time in vitro platelet function Thrombocytopenia Functional platelet defect or anti‐platelet drugs
PFA in vitro platelet function Aspirin, clopidogrel, or functional platelet disorder

      ITP in adults, unlike in childhood, seldom remits spontaneously. The initial treatment is with prednisolone 1 mg/kg daily or intravenous immunoglobulin 1.0 g/kg daily for two days. In patients with diabetes or renal impairment, an IvIg free from sucrose should be used. The condition is usually steroid‐responsive but frequently steroid‐dependent, and attempts to withdraw the steroids result in recurrence of thrombocytopenia. Often, the platelet count will stabilize at an acceptable level of above 50 × 109/l on no steroids or only a minimal dose, and in the absence of symptoms, this is often well tolerated for many years. If there is no response to steroids or an unacceptably high dose is required to maintain a satisfactory platelet count, alternative therapies include intravenous immunoglobulin, which usually raises the platelet count for around three weeks and sometimes results in a sustained remission, or the new agents that mimic thrombopoietin (TPO), the endogenous hormone that drives platelet production. Romiplostim is given by weekly injection and the dose titrated to produce a safe platelet count, while Eltrombopag is given orally daily with dose titration. Once the correct dosage is achieved, these drugs are given for 12 months; then the dose is reduced to see if remission has been achieved, which occurs in over 50% of cases. Splenectomy – which, although it does not prevent autoantibody production, does prevent premature platelet destruction by the spleen – is reserved for the most refractory cases, as it requires surgical intervention, although a laparoscopic splenectomy is far less invasive than an open splenectomy. A splenectomy successfully achieves complete remission in about 50–75% of cases progressing as far as surgery. However, splenectomy should not be undertaken lightly, as it is not without hazard, particularly in the thrombocytopenic patient. In addition to the operative risks, there is the risk of subsequent overwhelming post‐splenectomy sepsis: preoperative pneumococcal, Haemophilus


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