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Sarah Pett

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This is the current revision of this page, as edited by Kj cheetham (talk | contribs) at 19:54, 10 July 2024 (removed Category:Women in science and technology using HotCat. Not appropriate cat for bios.). The present address (URL) is a permanent link to this version.

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Sarah Pett
Alma materUniversity of Edinburgh
Scientific career
FieldsImmunopathology
InstitutionsUniversity of New South Wales
University College London

Sarah L. Pett is a Professor of Infectious Diseases at University College London. Pett is interested in the immunopathology of infections and the development of optimised treatment pathways for infections. During the COVID-19 pandemic, Pett led a clinical trial that investigated the efficacy of remdesivir as a treatment for coronavirus disease.[1]

Research and career

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In 2000 Pett joined the Kirby Institute in New South Wales, where she led international randomized controlled trials.[2][3] In 2013 Pett joined the Medical Research Council Clinical Trials Unit at University College London. She was promoted to the Chair of the Infectious Diseases theme in 2016.[4]

During the COVID-19 pandemic Pett led the Adaptive COVID-19 Treatment Trial (ACTT-EU/UK), a clinical trial into the efficacy of remdesivir as a treatment from coronavirus disease. Adult inpatients were given remdesivir or a placebo through a drip for up to ten days of their stay in hospital.[5] Pett showed that patients treated with remdesivir recovered 31% faster than those who did not receive treatment.[5]

She has also been involved in research on the neurological complications from COVID-19 and the co-morbid conditions that it may induce.[6]

Selected publications

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  • Neuhaus, Jacqueline Jacobs, David R. Baker, Jason V. Calmy, Alexandra Duprez, Daniel La Rosa, Alberto Kuller, Lewis H. Pett, Sarah L. Ristola, Matti Ross, Michael J. Shlipak, Michael G. Tracy, Russell Neaton, James D. (2010). "Markers of Inflammation, Coagulation, and Renal Function Are Elevated in Adults with HIV Infection". The Journal of Infectious Diseases. 201 (12): 1788–1795. doi:10.1086/652749. OCLC 999829131. PMC 2872049. PMID 20446848.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  • Babiker, Abdel G Emery, Sean Fätkenheuer, Gerd Gordin, Fred M Grund, Birgit Lundgren, Jens D Neaton, James D Pett, Sarah L Phillips, Andrew Touloumi, Giota Vjechaj, Michael J (2013). "Considerations in the rationale, design and methods of the Strategic Timing of AntiRetroviral Treatment (START) study". Clinical Trials (London, England). 10 (1 Suppl): S5–S36. doi:10.1177/1740774512440342. OCLC 870252553. PMC 3664112. PMID 22547421.{{cite journal}}: CS1 maint: multiple names: authors list (link)
  • Seddiki, Nabila; Sasson, Sarah C.; Santner‐Nanan, Brigitte; Munier, Meeling; Bockel, David van; Ip, Susanna; Marriott, Debbie; Pett, Sarah; Nanan, Ralph; Cooper, David A.; Zaunders, John J. (2009). "Proliferation of weakly suppressive regulatory CD4+ T cells is associated with over-active CD4+ T-cell responses in HIV-positive patients with mycobacterial immune restoration disease". European Journal of Immunology. 39 (2): 391–403. doi:10.1002/eji.200838630. ISSN 1521-4141. PMID 19180462. S2CID 24793084.

References

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  1. ^ UCL (2020-04-02). "UCL researchers lead trial to test remdesivir drug on COVID-19 patients". UCL News. Retrieved 2024-06-17.
  2. ^ "Sarah Pett". MRC Clinical Trials Unit at UCL. Retrieved 2020-05-15.
  3. ^ "Dr Sarah Pett". UNSW Sites. Retrieved 2024-06-17.
  4. ^ "Sarah Pett". MRC Clinical Trials Unit at UCL. Retrieved 2024-06-17.
  5. ^ a b "ACTT-EU/UK trial finds remdesivir speeds up COVID-19 recovery". MRC Clinical Trials Unit at UCL. Retrieved 2020-05-15.
  6. ^ "COVID-19 Tied to Wide Range of Neuropsychiatric Complications". Medscape. Retrieved 2024-06-17.