M.S. Losowsky
St James's University Hospital
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Featured researches published by M.S. Losowsky.
Clinica Chimica Acta | 1975
Marion J. Sheltawy; M.S. Losowsky
Abstract A relatively simple, cheap reliable method for determining faecal bile acids, using 3α-hydroxy steroid dehydrogenase is presented. Good recoveries were obtained even in the presence of very high fat concentrations. The mean value for a group of patients without gastrointestinal disease is reported.
British Journal of Haematology | 1995
Rashida Anwar; Alistair Stewart; Krzysztof J. A. Miloszewski; M.S. Losowsky; Alexander F. Markham
Summary. Factor XIII (FXIII) is a zymogen essential for normal haemostasis. In inherited FXIII deficiency the majority of cases show absence of the FXHIa subunit. Molecular analysis of PCR‐amplified FXIIIa subunit exonic regions, and of RT‐PCR amplified cDNA from six patients with FXIIIa subunit deficiency, from five unrelated families, has revealed 10 sequence changes: three mutations resulting in abnormal splicing of pre‐mRNA, one nonsense mutation, one deletion/insertion change, three point mutations producing Val34Leu, Asn60Lys and Arg408Gln changes, and two silent mutations. In three families the patients are homozygous for a specific deficiency causing mutation, and patients from the remaining two families are compound heterozygotes. Understanding the molecular pathology of the disorder provides insights into the structure‐function relationships of the various domains within the FXm protein. From a clinical point of view, it enables direct diagnosis at the DNA level and may aid the development of FXIII analogues to promote wound healing.
British Journal of Haematology | 1977
M.S. Losowsky; Krzysztof J. A. Miloszewski
In 1944 Robbins showed that the action of thrombin on purified fibrinogen, in the presence of calcium ions, produces a clot which is zelatively soluble, unless a small amount of plasma is also present. The factor responsible for the formation of insoluble clot is now known as factor XIII. This term is replacing others, the most popular of which has been Fibrin Stabilizing Factor (FSF). The first convincing demonstration of disease related to factor XI11 was the description of congenital, inherited deficiency by Duckert et a f in 1960.
Acta Haematologica | 1984
Fear Jd; Krzysztof J. A. Miloszewski; M.S. Losowsky
A patient with an acquired inhibitor to factor XIII is reported. The patients plasma produced a profound inhibition of factor XIII activity in normal plasma measured by a dansylcadaverine casein assay and stimulated a very abnormal pattern of fibrin cross-linking, not normally seen with factor XIII. Partial characterisation of the inhibitor suggests that it is heat stable and not an immunoglobulin.
Acta Haematologica | 1974
Krzysztof J. A. Miloszewski; M.J. Sheltawy; M.S. Losowsky
Factor XIII levels are within the normal range in patients with pathological fibrinolysis and remain unchanged in the intense fibrinolytic state induced by streptokinase infusion. Incubation of plasma
Annals of Nutrition and Metabolism | 1975
Marion J. Sheltawy; M.S. Losowsky
Malabsorption of fat and α-tocopherol was induced in rats by feeding cholestyramine and the effect of Tween 80 and Pluronic F 68 was assessed. Tween 80 did not influence the malabsorption of fat or α-
Acta Haematologica | 1974
Krzysztof J. A. Miloszewski; M.J. Sheltawy; M.S. Losowsky
The effect of fibrinogen/fibrin degradation products (FDP) on the stabilisation of fibrin was tested in vitro by the clot solubility assay and by the transamidase assay of 14
Hepatology | 1991
J. Hilary Green; Peter N. Bramley; M.S. Losowsky
Archive | 1994
Richard Heatley; J. Hilary Green; M.S. Losowsky
Thrombosis et diathesis haemorrhagica | 1972
Marion Sheltawy; Krzysztof J. A. Miloszewski; M.S. Losowsky