Claire Crossan scite author profile

Acellular materials of xenogenic origin are used worldwide as xenografts and Phase I trials of viable pig pancreatic islets are currently being performed. However, limited information is available on transmission of porcine endogenous retrovirus (PERV) after xenotransplantation and on the long-term immune response of recipients to xenoantigens. We analyzed the blood of burn patients who had received living pig skin dressings for up to 8 weeks for the presence of PERV as well as for the level and nature of their long term (maximum 34 years) immune response against pig antigens. Whilst no evidence of PERV genomic material or anti PERV antibody response was found, we observed a moderate increase in anti αGal antibodies and a high and sustained anti non-αGal IgG response in those patients. Antibodies against the non-human sialic acid Neu5Gc constituted the anti non-αGal response with the recognition pattern on a sialogly can array differing from that of burn patients treated without pig skin. These data suggest that anti-Neu5Gc antibodies may represent a barrier for long-term acceptance of porcine xenografts. As anti-Neu5Gc antibodies can promote chronic inflammation, the long-term safety of living and acellular pig tissue implants in recipients warrants further evaluation.

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Hepatitis E virus in Scottish blood donors

Cleland

et al. 2013

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Hepatitis E Virus Genotype 3 in Shellfish, United Kingdom

Crossan¹,

Baker²,

Craft³

et al. 2012

Emerg. Infect. Dis.

139

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Review article: hepatitis E—a concise review of virology, epidemiology, clinical presentation and therapy

Donnelly

Scobie

Crossan

et al. 2017

Aliment Pharmacol Ther

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SummaryBackground: Hepatitis E virus (HEV) is a leading cause of acute icteric hepatitis and acute liver failure in the developing world. During the last decade, there has been increasing recognition of autochthonous (locally acquired) HEV infection in developed countries. Chronic HEV infection is now recognised, and in transplant recipients this may lead to cirrhosis and organ failure.Aim: To detail current understanding of the molecular biology of HEV, diagnostic and therapeutic strategies and propose future directions for basic science and clinical research.Methods: PubMed was searched for English language articles using the key words "hepatitis E", "viral hepatitis", "autochthonous infection", "antiviral therapy", "liver transplantation", "acute", "chronic", "HEV", "genotype", "transmission" "food-borne", "transfusion". Additional relevant publications were identified from article reference lists. Future work should focus on increasing awareness of HEV infection in the developed world, emphasising the need for clinicians to have a low threshold for HEV testing, particularly in immunosuppressed patients. Patients at potential risk of chronic HEV infection must also be educated and given advice regarding prevention of infection.

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Hepatitis E virus in patients with decompensated chronic liver disease: a prospective UK/French study

Blasco-Perrin

Madden

Stanley

et al. 2015

Aliment Pharmacol Ther

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Claire Crossan

Long-Term IgG Response to Porcine Neu5Gc Antigens without Transmission of PERV in Burn Patients Treated with Porcine Skin Xenografts

Hepatitis E virus in Scottish blood donors

Hepatitis E Virus Genotype 3 in Shellfish, United Kingdom

Review article: hepatitis E—a concise review of virology, epidemiology, clinical presentation and therapy

Hepatitis E virus in patients with decompensated chronic liver disease: a prospective UK/French study

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