Your search keyword '"Christopher A. Ludlam"' showing total 5 results

1. Clinical perspectives of emerging pathogens in bleeding disorders

Author

Michael P. Diamond, Samuel A. Bozzette, Peter Simmonds, Mario von Depka, Michael L. Tapper, Marion A. Koerper, Bruce Ritchie, Jamie E. Siegel, Samuel L. Stanley, Roshni Kulkarni, William G. Powderly, and Christopher A. Ludlam

Subjects

Human immunodeficiency virus (HIV), Hemophilia A, medicine.disease_cause, Communicable Diseases, Emerging, Communicable Diseases, Medical and Health Sciences, Article, Virus, General & Internal Medicine, medicine, Animals, Humans, Blood plasma fractionation, Emerging, Transmission (medicine), business.industry, General Medicine, Hepatitis B, medicine.disease, Virology, Blood Coagulation Factors, Safety profile, Viruses, Genetic selection, Blood-Borne Pathogens, Public Health, business

Abstract

Summary As a result of immunological and nucleic-acid screening of plasma donations for transfusion-transmissible viruses, and the incorporation of viral reduction processes during plasma fractionation, coagulation-factor concentrates (CFC) are now judged safe in terms of many known infectious agents, including hepatitis B and C viruses, HIV, and human T-cell lymphotropic virus. However, emerging pathogens could pose future threats, particularly those with blood-borne stages that are resistant to viral-inactivation steps in the manufacturing process, such as non-lipid-coated viruses. As outlined in this Review, better understanding of infectious diseases allows challenges from newly described agents of potential concern in the future to be anticipated, but the processes of zoonotic transmission and genetic selection or modification ensure that plasma-derived products will continue to be subject to infectious concerns. Manufacturers of plasma-derived CFC have addressed the issue of emerging infectious agents by developing recombinant products that limit the need for human plasma during production. Such recombinant products have extended the safety profile of their predecessors by ensuring that all reagents used for cell culture, purification steps, and stabilisation and storage buffers are completely independent of human plasma.

Published

2006

2. Detection of a novel DNA virus (TT virus) in blood donors and blood products

Author

C Lycett, JA Ellender, Lisa Jarvis, P L Yap, Peter Simmonds, Christopher A. Ludlam, D M MacDonald, J Gillon, L E Prescott, Geoffrey Haydon, and F Davidson

Subjects

Adult, Male, medicine.medical_specialty, Torque teno virus, Hepatitis, Viral, Human, Hepatitis C virus, Population, Blood Component Transfusion, Blood Donors, Biology, Hemophilia A, medicine.disease_cause, Polymerase Chain Reaction, Virus, Transfusion transmitted virus, Japan, Internal medicine, medicine, Humans, Viremia, Child, education, Aged, Hepatitis, Clotting factor, education.field_of_study, Hematology, DNA Viruses, General Medicine, Middle Aged, medicine.disease, biology.organism_classification, Virology, United Kingdom, Hepatic Encephalopathy, Immunology, Female

Abstract

Summary Background A newly discovered DNA virus, transfusion- transmitted virus (TTV), has been implicated as a cause of post-transfusion hepatitis. We investigated the frequency of TTV viraemia in UK blood donors, and the extent to which TTV contaminates blood products such as factor VIII and IX clotting factors. We also investigated the possible aetiological role of TTV in cryptogenic fulminant hepatic failure (FHF). Methods We extracted DNA from plasma of blood donors and patients with FHF, and from blood products (factor VIII and IX clotting-factor concentrates, immunoglobulin preparations). We detected TTV by PCR using primers from a conserved region in the TTV genome. Findings TTV viraemia was detected in 19 (1·9%) of 1000 non-remunerated regular blood donors. Infection occurred more frequently in older donors (mean age 53 years), compared with the age prolife of donors infected with hepatitis C virus and other parenterally-transmitted viruses. TTV contamination was found in ten (56%) of 18 batches of factor VIII and IX concentrate manufactured from such non- remunerated donors, and in seven (44%) of 16 batches of commercially available products. Whereas solvent or detergent treatment had little effect on the detection of TTV in factor VIII and IX by PCR, this virucidal step seemed to inactivate TTV infectivity. TTV infection was detected in four (19%) of 21 patients with FHF; in three cases, infection was detected at the onset of disease and could thus not be excluded from its aetiology. Interpretation TTV viraemia is frequent in the blood-donor population, and transmission of TTV through transfusion of blood components may have occurred extensively. Clinical assessment of infected donors and recipients of blood and blood products, and assessment of TTV's aetiological role in hepatic and extra-hepatic disease, are urgently needed.

Published

1998

3. Mortality from liver cancer and liver disease in haemophilic men and boys in UK given blood products contaminated with hepatitis C

Author

Geoffrey Dusheiko, Christine A. Lee, R. J. D. Spooner, Christopher A. Ludlam, Paul L. F. Giangrande, D. W. Ewart, Charles R. Rizza, Sarah C. Darby, and F. Eric Preston

Subjects

medicine.medical_specialty, education.field_of_study, Blood transfusion, business.industry, medicine.medical_treatment, Population, General Medicine, Hepatitis C, Haemophilia, medicine.disease, Liver disease, Internal medicine, Hepatocellular carcinoma, Immunology, Medicine, business, Liver cancer, education, Cause of death

Abstract

Summary Background Most people with haemophilia who were treated with blood products before the introduction of virus-inactivation procedures were infected with the hepatitis-C virus (HCV). However, there is little quantitative information about the long-term effects on mortality of such infection. Methods We carried out a cohort study of mortality from liver cancer and liver disease in 4865 haemophilic men and boys in the UK. They were treated between 1969 and 1985 with blood products carrying a high risk of HCV infection, and were followed up from first recorded exposure to Jan 1, 1993. Findings Based on death-certificate information, mortality was 16·7 times higher than in the general population for liver disease (95% CI 12·5–22·0; 51 deaths), and 5·6 times higher (1·8–13·0; five deaths) for liver cancer. For men and boys with severe haemophilia who were not infected with HIV-1, the cumulative risks of death from chronic or unspecified liver disease or from liver cancer in the 25 years since first recorded exposure to high HCV-risk products were 1·4% (0·7–3·0) at all ages, and 0·10% (0·01–0·7), 2·2% (0·8–6·1), and 14·3% (4·5–40·9) for those with first recorded exposure at ages under 25, 25–44, and 45 or older. For those with haemophilia and HIV-1 infection, the corresponding risks were 6·5% (4·5–9·5) at all ages, and 3·8% (2·1–6·8), 17·1% (10·0–28·5), and 18·7% (6·4–47·6) in the three age-groups. In those with severe haemophilia, age-standardised all-cause mortality was stable during 1969–84 but increased during 1985–92 in both HIV-1-infected and HIV-1-uninfected groups. Among those not infected with HIV-1, the increase in all-cause mortality resulted largely from deaths attributed to chronic or unspecified liver disease or liver cancer in men aged over 45. Interpretation There is an emerging risk of mortality from liver disease and liver cancer in the UK haemophilia population in individuals both infected and uninfected with HIV-1, which probably results from infection with hepatitis C.

Published

1997

4. Prothrombin time to assess fulminant hepatic failure

Author

Neil C. Henderson, Philip N. Newsome, Kenneth J. Simpson, Christopher A. Ludlam, and Lorna Germain

Subjects

Prothrombin time, medicine.medical_specialty, medicine.diagnostic_test, business.industry, General Medicine, Prognosis, Gastroenterology, Fulminant hepatic failure, Internal medicine, Prothrombin Time, Humans, Medicine, Prospective Studies, Reagent Kits, Diagnostic, business, Prospective cohort study, Liver Failure

Published

2001

5. Confirmation of non-infection in persistently HIV-seronegative recipients of contaminated factor VIII

Author

John F. Peutherer, S Rebus, P Barr, Michael Steel, Christopher A. Ludlam, and Henry G. Watson

Subjects

Factor VIII, Time Factors, business.industry, Human immunodeficiency virus (HIV), General Medicine, HIV Antibodies, medicine.disease_cause, Polymerase Chain Reaction, Virology, Cohort Studies, Immunoglobulin M, HIV Seropositivity, Humans, Medicine, Drug Contamination, business

Published

1990