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Xiaosong Liu

Researcher at University of the Sunshine Coast

Publications -  50
Citations -  1520

Xiaosong Liu is an academic researcher from University of the Sunshine Coast. The author has contributed to research in topics: Immune system & Cytotoxic T cell. The author has an hindex of 23, co-authored 50 publications receiving 1307 citations. Previous affiliations of Xiaosong Liu include Princess Alexandra Hospital & University of Queensland.

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Journal ArticleDOI

The Dosage of the Derivative of Clostridium Ghonii (DCG) Spores Dictates Whether an IFNγ/IL-9 or a Strong IFNγ Response Is Elicited in TC-1 Tumour Bearing Mice.

TL;DR: Intravenous administration of the derivative of Clostridial ghonii (DCG) spores leads to both tumour and systemic inflammatory responses characterized by increased IFNγ/IL-9 secreting T cells in the spleen and the tumour.
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Mucosal Immunisation with Papillomavirus Virus-like Particles Elicits Systemic and Mucosal Immunity in Mice

TL;DR: It is concluded that immunisation with papillomavirus VLPs via mucosal and intramuscular routes, without adjuvant, can elicit specific antibody at mucosal surfaces and also systemic VLP epitope specific T cell responses.
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Host immune responses to the itch mite, Sarcoptes scabiei, in humans

TL;DR: A better understanding is provided of human immune responses to S. scabiei in ordinary and crusted scabies phenotypes to provide a better understanding of the significant global impact of the disease.
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The role of interferon gamma in regulation of CD4+ T-cells and its clinical implications.

TL;DR: Its target T-regulatory cells may be used for the clinical treatment of autoimmune diseases and future study could also focus on promotion of the beneficial effects of IFNgamma and blocking those unwanted IFNGamma-induced activities.
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Despite differences between dendritic cells and Langerhans cells in the mechanism of papillomavirus-like particle antigen uptake, both cells cross-prime T cells.

TL;DR: Compared HPV-VLP uptake mechanisms in human monocyte-derived DC and LC, and their ability to cross-present HPV VLP-associated antigen in the MHC class I pathway are compared to suggest fundamentally different routes of VLP uptake by DC andLC.