期刊
ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS
卷 483, 期 1, 页码 120-126出版社
ELSEVIER SCIENCE INC
DOI: 10.1016/j.abb.2008.12.006
关键词
Paracentrotus lividus; Amyloid-beta; Oligomers; Fibrillar aggregates; Apoptosis; Animal model
Alzheimer's disease (AD) is the most common form of dementia. The Cause of AD is closely related to the accumulation of amyloid beta peptide in the neuritic plaques. The use of animal model systems represents a good strategy to elucidate the molecular mechanism behind the development of this pathology. Here we use the Paracentrotus lividus embryo to identify molecules and pathways that can be involved in the degenerative process. As a first step, we identified the presence of an antigen related to the human APP, called PlAPP. This antigen, after gastrula stage, is processed producing a polypeptide of about 10 kDa. By immunohistochemistry we localized the PlAPP antigen in some serotonin expressing cells. Similarly, after 48 or 96 h incubation, a recombinant beta-amyloid peptide, rA beta 42, accumulates around the intestinal tube and oesophagus. In addition, incubation of sea urchin embryos with two different solutions rich in oligomers and fibrillar aggregates of rA beta 42 induce activation of apoptosis as detected by TUNEL assay. Moreover, we demonstrate that aggregates induce apoptosis by extrinsic pathway activation, whereas oligomers induce apoptosis both by extrinsic and intrinsic pathway activation. Utilizing an apoptotic inhibitor, caspases activation was offset and morphological damage rescued. Taken together all these observations suggest that the sea urchin may be a simple and suitable model to characterize the mechanism underlining the cytotoxicity of A beta 42. (C) 2009 Elsevier Inc. All rights reserved.
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