Haematology - Barbara J. Bain

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showing hypocellularity with reduction of haemopoietic activity around the marrow fat spaces (top images, H&E) (all images ×50 objective). The hypocellular areas show preserved architecture and an amorphous myxoid (mucoid) interstitium. Subsequent staining with Alcian blue (bottom left and centre) and periodic acid–Schiff (bottom right) confirmed the diagnosis of gelatinous transformation, also known as myxoid degeneration.

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      Typically, this condition involves the marrow diffusely (above left, H&E and right, Alcian blue ×50), resulting in peripheral blood cytopenias with neutropenia and anaemia being most frequent. Gelatinous transformation of the bone marrow is an important condition to recognise and should not be mistaken for marrow aplasia or marrow necrosis. It is typically seen as part of the catabolic response to chronic debilitating disease (malignant or non‐malignant) and/or malnutrition. The condition will regress on treating the underlying cause.

      1 Myxoid degeneration (gelatinous transformation) can be a feature of:Acquired immune deficiency syndromeAnorexia nervosaExtreme exerciseMetastatic carcinomaMorbid obesityFor answers and discussion, see page 206.

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      A 50‐year‐old man with a progressive myopathy and cardiomyopathy was referred to a neurologist because of early cognitive decline and tic‐like involuntary movements. His full blood count was normal but a blood film was requested. This showed prominent acanthocytes; these are dense cells with prominent cytoplasmic projections (spicules), which are irregular in length and shape (acanthus is Greek for ‘thorny’) (left images ×100 objective). Routine renal and liver biochemistry and serum lipids were normal. A diagnosis of McLeod syndrome was considered and confirmed when a mutation in the XK gene at Xp21.1 was identified. McLeod syndrome is an X‐linked multisystem disorder, being one of a number of the rare neuroacanthocytic disorders. The condition is characterised by acanthocytosis, mild compensated haemolysis, weak expression of Kell blood group antigens, myopathy, cardiomyopathy and progressive neurological decline with cognitive impairment, involuntary movements, seizures and peripheral neuropathy. Peripheral blood morphology may provide a useful pointer to the diagnosis, as in this case.

      A third patient, a 32‐year‐old man with malnutrition from severe exocrine pancreatic insufficiency of unknown aetiology was hospitalised with a respiratory infection. He was poorly compliant with pancreatic enzyme supplements and appeared ill, grossly malnourished and wasted. His full blood count showed Hb 109 g/l, MCV 86.5 fl, MCH 26.3 pg, WBC 6.2 × 109/l and platelets 218 × 109/l. Serum ferritin was low at 9 μg/l and a blood film was requested. This showed significant hypochromia, consistent with iron deficiency, but also marked acanthocytosis with some of these cells appearing very dense (right images ×100). His lipid profile was abnormal, showing total cholesterol 2.2 mmol/l (optimal <5.2), triglycerides 0.8 mmol/l (NR 0.2–2.3), high‐density lipoprotein 0.6 mmol/l (optimal >1), LDL 1.2 mmol/l (optimal <2.59) and VLDL 0.4 mmol/l (NR 0.1–1.7). Serum apolipoprotein B levels were 0.6 g/l (NR 0.6–1.3) and screening for mutation in MTTP was negative. A diagnosis of acquired acanthocytosis, with iron deficiency secondary to severe lipid malabsorption from pancreatic exocrine failure was made.

      1 Acanthocytes in a blood film can be the result of:Anorexia nervosaLiver failureSplenectomyStorage artefactTransfusion of blood at the end of its shelf lifeFor answers and discussion, see page 206.

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      A 53‐year‐old man with rheumatoid arthritis was referred on account of progressive neutropenia whilst on weekly methotrexate therapy. Importantly, the methotrexate was withheld but the neutropenia continued and in fact worsened. At the time of referral the full blood count showed Hb 159 g/l, WBC 6.5 × 109/l, neutrophils 0.6 × 109/l, lymphocytes 5.1 × 109/l and platelets 133 × 109/l. The lymphocytosis had actually evolved during the period when methotrexate was suspended. The blood film showed prominent large granular lymphocytes (top images ×100 objective) and on immunophenotyping these expressed CD8, weak CD5, CD2, CD3 and CD57, whilst expression of CD7 and CD26 was lost, suggesting a clonal T‐cell disorder. The bone marrow trephine biopsy sections showed a cellular marrow with a subtle interstitial (bottom left, H&E ×50) and intrasinusoidal (CD3, bottom centre and right, immunoperoxidase ×50) T‐cell infiltrate. T‐cell receptor gene rearrangement studies showed a clonal population, and sequencing of STAT3 and STAT5B genes showed a gain of function mutation in STAT3, Y640F, which has been associated with a therapeutic response to methotrexate. The clinical advice was therefore to restart methotrexate treatment. This resulted in improvement in rheumatic symptoms but also in resolution of lymphocytosis and neutropenia: Hb 160 g/l, WBC 5.0 × 109/l, neutrophils 2.1 × 109/l, lymphocytes 2.9 × 109/l and platelets 162 × 109/l.

      1 T‐cell large granular lymphocytic leukaemia:Can lead to anaemia due to pure red cell aplasia or autoimmune haemolytic anaemiaHas specific diagnostic features on trephine biopsyShows an association with Felty syndromeShows an association with thymomaTypically shows expression of CD3, CD8 and CD57For answers and discussion, see page 206.

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      A 40‐year‐old, previously fit man presented with progressive fatigue. Physical examination showed pallor and mild icterus. His full blood count showed Hb 87 g/l, WBC 1.7 × 109/l, neutrophils 0.8 × 109/l and platelets 26 × 109/l. His blood film showed no specific features but, importantly, red cell fragments, spherocytes and blast cells were not seen. Serum bilirubin and LDH were both mildly elevated. A direct Coombs

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