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Your search keyword '"Fu, Amy K. Y."' showing total 5 results
Start Over Author "Fu, Amy K. Y." Publication Type Electronic Resources
5 results on '"Fu, Amy K. Y."'

1. A blood-based multi-pathway biomarker assay for early detection and staging of Alzheimer's disease across ethnic groups

Author

Jiang, Yuanbing, Uhm, Hyebin, Ip, Fanny C., Ouyang, Li, Lo, Ronnie M. N., Cheng, Elaine Y. L., Cao, Xiaoyun, Tan, Clara M. C., Law, Brian C. H., Ortiz-Romero, Paula, Puig-Pijoan, Albert, Fernández-Lebrero, Aida, Contador, José, Mok, Kin Ying Boniface, Hardy, John, Kwok, Timothy C. Y., Mok, Vincent C. T., Suárez-Calvet, Marc, Zetterberg, Henrik, Fu, Amy K. Y., Ip, Nancy Yuk-yu, Jiang, Yuanbing, Uhm, Hyebin, Ip, Fanny C., Ouyang, Li, Lo, Ronnie M. N., Cheng, Elaine Y. L., Cao, Xiaoyun, Tan, Clara M. C., Law, Brian C. H., Ortiz-Romero, Paula, Puig-Pijoan, Albert, Fernández-Lebrero, Aida, Contador, José, Mok, Kin Ying Boniface, Hardy, John, Kwok, Timothy C. Y., Mok, Vincent C. T., Suárez-Calvet, Marc, Zetterberg, Henrik, Fu, Amy K. Y., and Ip, Nancy Yuk-yu

Abstract

INTRODUCTION: Existing blood-based biomarkers for Alzheimer's disease (AD) mainly focus on its pathological features. However, studies on blood-based biomarkers associated with other biological processes for a comprehensive evaluation of AD status are limited. METHODS: We developed a blood-based, multiplex biomarker assay for AD that measures the levels of 21 proteins involved in multiple biological pathways. We evaluated the assay's performance for classifying AD and indicating AD-related endophenotypes in three independent cohorts from Chinese or European-descent populations. RESULTS: The 21-protein assay accurately classified AD (area under the receiver operating characteristic curve [AUC] = 0.9407 to 0.9867) and mild cognitive impairment (MCI; AUC = 0.8434 to 0.8945) while also indicating brain amyloid pathology. Moreover, the assay simultaneously evaluated the changes of five biological processes in individuals and revealed the ethnic-specific dysregulations of biological processes upon AD progression. DISCUSSION: This study demonstrated the utility of a blood-based, multi-pathway biomarker assay for early screening and staging of AD, providing insights for patient stratification and precision medicine. HIGHLIGHTS: The authors developed a blood-based biomarker assay for Alzheimer's disease. The 21-protein assay classifies AD/MCI and indicates brain amyloid pathology. The 21-protein assay can simultaneously assess activities of five biological processes. Ethnic-specific dysregulations of biological processes in AD were revealed. © 2024 The Authors. Alzheimer's & Dementia published by Wiley Periodicals LLC on behalf of Alzheimer's Association.

Published
2024

2. Brain-wide Cas9-mediated cleavage of a gene causing familial Alzheimer’s disease alleviates amyloid-related pathologies in mice

Author

Duan, Yangyang, Ye, Tao, Qu, Zhe, Chen, Yuewen, Miranda, Abigail, Zhou, Xiaopu, Lok, Ka-Chun, Chen, Yu, Fu, Amy K. Y., Gradinaru, Viviana, Ip, Nancy Y., Duan, Yangyang, Ye, Tao, Qu, Zhe, Chen, Yuewen, Miranda, Abigail, Zhou, Xiaopu, Lok, Ka-Chun, Chen, Yu, Fu, Amy K. Y., Gradinaru, Viviana, and Ip, Nancy Y.

Abstract

The pathology of familial Alzheimer’s disease, which is caused by dominant mutations in the gene that encodes amyloid-beta precursor protein (APP) and in those that encode presenilin 1 and presenilin 2, is characterized by extracellular amyloid plaques and intracellular neurofibrillary tangles in multiple brain regions. Here we show that the brain-wide selective disruption of a mutated APP allele in transgenic mouse models carrying the human APP Swedish mutation alleviates amyloid-beta-associated pathologies for at least six months after a single intrahippocampal administration of an adeno-associated virus that encodes both Cas9 and a single-guide RNA that targets the mutation. We also show that the deposition of amyloid-beta, as well as microgliosis, neurite dystrophy and the impairment of cognitive performance, can all be ameliorated when the CRISPR–Cas9 construct is delivered intravenously via a modified adeno-associated virus that can cross the blood–brain barrier. Brain-wide disease-modifying genome editing could represent a viable strategy for the treatment of familial Alzheimer’s disease and other monogenic diseases that affect multiple brain regions.

Published
2021

3. Increased Axin expression enhances adult hippocampal neurogenesis and exerts an antidepressant effect

Author

Chen, Weiwei LIFS, Fu, Wing Yu, Su, Yiting, Fang, Weiqun, Fu, Amy K. Y., Ip, Nancy Yuk-yu, Chen, Weiwei LIFS, Fu, Wing Yu, Su, Yiting, Fang, Weiqun, Fu, Amy K. Y., and Ip, Nancy Yuk-yu

Abstract

Major depressive disorders are emerging health problems that affect millions of people worldwide. However, treatment options and targets for drug development are limited. Impaired adult hippocampal neurogenesis is emerging as a key contributor to the pathology of major depressive disorders. We previously demonstrated that increasing the expression of the multifunctional scaffold protein Axis inhibition protein (Axin) by administration of the small molecule XAV939 enhances embryonic neurogenesis and affects social interaction behaviors. This prompted us to examine whether increasing Axin protein level can enhance adult hippocampal neurogenesis and thus contribute to mood regulation. Here, we report that stabilizing Axin increases adult hippocampal neurogenesis and exerts an antidepressant effect. Specifically, treating adult mice with XAV939 increased the amplification of adult neural progenitor cells and neuron production in the hippocampus under both normal and chronic stress conditions. Furthermore, XAV939 injection in mice ameliorated depression-like behaviors induced by chronic restraint stress. Thus, our study demonstrates that Axin/XAV939 plays an important role in adult hippocampal neurogenesis and provides a potential therapeutic approach for mood-related disorders.

Published
2019

4. Increased Axin expression enhances adult hippocampal neurogenesis and exerts an antidepressant effect

Author

Chen, Weiwei LIFS, Fu, Wing Yu, Su, Yiting, Fang, Weiqun, Fu, Amy K. Y., Ip, Nancy Yuk-yu, Chen, Weiwei LIFS, Fu, Wing Yu, Su, Yiting, Fang, Weiqun, Fu, Amy K. Y., and Ip, Nancy Yuk-yu

Abstract

Major depressive disorders are emerging health problems that affect millions of people worldwide. However, treatment options and targets for drug development are limited. Impaired adult hippocampal neurogenesis is emerging as a key contributor to the pathology of major depressive disorders. We previously demonstrated that increasing the expression of the multifunctional scaffold protein Axis inhibition protein (Axin) by administration of the small molecule XAV939 enhances embryonic neurogenesis and affects social interaction behaviors. This prompted us to examine whether increasing Axin protein level can enhance adult hippocampal neurogenesis and thus contribute to mood regulation. Here, we report that stabilizing Axin increases adult hippocampal neurogenesis and exerts an antidepressant effect. Specifically, treating adult mice with XAV939 increased the amplification of adult neural progenitor cells and neuron production in the hippocampus under both normal and chronic stress conditions. Furthermore, XAV939 injection in mice ameliorated depression-like behaviors induced by chronic restraint stress. Thus, our study demonstrates that Axin/XAV939 plays an important role in adult hippocampal neurogenesis and provides a potential therapeutic approach for mood-related disorders.

Published
2019

5. Increased Axin expression enhances adult hippocampal neurogenesis and exerts an antidepressant effect

Author

Chen, Weiwei LIFS, Fu, Wing Yu, Su, Yiting, Fang, Weiqun, Fu, Amy K. Y., Ip, Nancy Yuk-yu, Chen, Weiwei LIFS, Fu, Wing Yu, Su, Yiting, Fang, Weiqun, Fu, Amy K. Y., and Ip, Nancy Yuk-yu

Abstract

Major depressive disorders are emerging health problems that affect millions of people worldwide. However, treatment options and targets for drug development are limited. Impaired adult hippocampal neurogenesis is emerging as a key contributor to the pathology of major depressive disorders. We previously demonstrated that increasing the expression of the multifunctional scaffold protein Axis inhibition protein (Axin) by administration of the small molecule XAV939 enhances embryonic neurogenesis and affects social interaction behaviors. This prompted us to examine whether increasing Axin protein level can enhance adult hippocampal neurogenesis and thus contribute to mood regulation. Here, we report that stabilizing Axin increases adult hippocampal neurogenesis and exerts an antidepressant effect. Specifically, treating adult mice with XAV939 increased the amplification of adult neural progenitor cells and neuron production in the hippocampus under both normal and chronic stress conditions. Furthermore, XAV939 injection in mice ameliorated depression-like behaviors induced by chronic restraint stress. Thus, our study demonstrates that Axin/XAV939 plays an important role in adult hippocampal neurogenesis and provides a potential therapeutic approach for mood-related disorders.

Published
2019

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