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    Home > Active Ingredient News > Study of Nervous System > Epimedicine: a specific protein associated with the development of ovarian cancer or may worsen neurodegeneration in patients with Alzheimer's disease

    Epimedicine: a specific protein associated with the development of ovarian cancer or may worsen neurodegeneration in patients with Alzheimer's disease

    • Last Update: 2020-01-19
    • Source: Internet
    • Author: User
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    January 19, 2020 / Biovalley BIOON / -- recently, in a research report published in the International Journal ebomedicine, scientists from Houston Methodist cancer center and other institutions identified a special protein in ovarian cancer, which may promote the decline of brain function and the occurrence of Alzheimer's disease Source: Houston Methodist researcher Stephen T.C According to Wong, our results show that one protein with known function may play another role, which may help to develop new strategies for disease treatment; researchers have revealed the different roles of β - amyloid protein in the pathogenesis of neurodegenerative diseases, and many scientists engaged in Alzheimer's disease research only focus on β - amyloid The association of proteins or β - amyloid with other proteins, such as tau In this study, the researchers revealed the new role of a protein called ociad1 (ovarian cancer immune response antigen domain contains 1 protein) The first researchers found that ociad1 is responsible for ovarian cancer metastasis and stem cells The protein can damage neurons and synapses in the brain, thus inducing neurodegeneration in Alzheimer's disease patients The researchers pointed out that this study solved a basic problem of Alzheimer's disease, that is, β - amyloid protein may appear 20 years before brain function declines, and this protein is involved in the occurrence of progressive neurodegeneration Analyzing the factors that promote the progressive decline of brain function in patients with Alzheimer's disease may help to develop new diagnostic biomarkers and new therapies The researchers combined computational methods with laboratory research to analyze brain tissue of the late Alzheimer's disease patients and mice models They found that ociad1 may play a key role in the progressive neurodegeneration of the disease by damaging the function of cell mitochondria As the energy factory of cells, the damage of mitochondria may lead to trickle cells in the brain The death effect can cause neuron damage Dr Xuping Li, researcher, said that we applied systems biology Now we have identified ociad1 as a new type of neurodegenerative factor Predicting its function can help us to determine whether ociad1 can mediate the long-term effect of β - amyloid protein in cells and the damage effect of synapse by damaging the function of mitochondria In general, Alzheimer's disease research focuses on several main topics, namely, the key role of amyloid protein in the process of neuron loss, and how the toxic protein can induce damage by interacting with tau protein; however, until recently, researchers thought that β amyloid protein might be a bystander, and they also questioned that it is Whether it can really induce neurodegenerative diseases In the next step, researchers want to clarify whether ociad1 plays a key role in the interaction of two known changes in Alzheimer's disease (β - amyloid protein and tau aggregation) If so, researchers may need to conduct additional research to clarify the potential of ociad1 as a biomarker or therapeutic target At present, Alzheimer's disease affects more than 5.8 million Americans, and with the increase of the aging population, the disease will become more popular According to the data of Alzheimer's disease association and American CDC, Alzheimer's disease is currently the most expensive disease to treat in the United States, and the treatment of the disease is expected to cost US $290 billion in 2019 Original source: Xuping Li et al, ociad1 contributions to neurogenesis in Alzheimer's disease by inducing mitochondria dysfunction, national vulnerability and synthetic images, ebiomedicine (2020) Doi: 10.1016/j.ebiom.2019.11.030
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