Targeting γ-secretase for familial Alzheimer’s disease
被引:0
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作者:
Michael S. Wolfe
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机构:University of Kansas,Department of Medicinal Chemistry
Michael S. Wolfe
机构:
[1] University of Kansas,Department of Medicinal Chemistry
来源:
Medicinal Chemistry Research
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2021年
/
30卷
关键词:
Proteolysis;
Amyloid;
Presenilin;
Activators;
D O I:
暂无
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学科分类号:
摘要:
Familial Alzheimer’s disease (FAD) is a rare early-onset genetic form of common dementia of old age. Striking in middle age, FAD is caused by missense mutations in three genes: APP (encoding the amyloid precursor protein) and PSEN1 and PSEN2 (encoding presenilin-1 and presenilin-2). APP is proteolytically processed successively by β-secretase and γ-secretase to produce the amyloid β-peptide (Aβ). Presenilin is the catalytic component of γ-secretase, a membrane-embedded aspartyl protease complex that cleaves APP within its single transmembrane domain to produce Aβ of varying lengths. Thus, all FAD mutations are found in the substrate and the enzyme that produce Aβ. The 42-residue variant Aβ42 has been the primary focus of Alzheimer drug discovery for over two decades, as this particular peptide is highly prone to aggregation, is the major protein deposited in the characteristic cerebral plaques of Alzheimer’s disease and is proportionately elevated in FAD. Despite extensive efforts, all agents targeting Aβ and Aβ42 have failed in the clinic, including γ-secretase inhibitors, leading to questioning of the amyloid hypothesis of Alzheimer pathogenesis. However, processing of the APP transmembrane domain by γ-secretase is complex, involving initial endoproteolysis followed by successive carboxypeptidase trimming steps to secreted Aβ peptides such as Aβ42. Recent findings reveal that FAD mutations in PSEN1 and in APP result in the deficient trimming of initially formed long Aβ peptides. A logical drug discovery strategy for FAD could therefore involve the search for compounds that rescue this deficient carboxypeptidase activity. The rare early-onset FAD arguably presents a simpler path to developing effective therapeutics compared to the much more complex heterogeneous sporadic Alzheimer’s disease.
机构:
Mahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Schaduangrat, Nalini
Prachayasittikul, Veda
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Mahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Prachayasittikul, Veda
Choomwattana, Saowapak
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机构:
Mahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Choomwattana, Saowapak
Wongchitrat, Prapimpun
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机构:
Mahidol Univ, Ctr Res & Innovat, Fac Med Technol, Bangkok, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Wongchitrat, Prapimpun
Phopin, Kamonrat
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Mahidol Univ, Ctr Res & Innovat, Fac Med Technol, Bangkok, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Phopin, Kamonrat
Suwanjang, Wilasinee
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机构:
Mahidol Univ, Ctr Res & Innovat, Fac Med Technol, Bangkok, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Suwanjang, Wilasinee
Malik, Aijaz Ahmad
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机构:
Mahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Malik, Aijaz Ahmad
Vincent, Bruno
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机构:
Mahidol Univ, Inst Mol Biosci, Bangkok 73170, Nakhon Pathom, Thailand
CNRS, Paris, FranceMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
Vincent, Bruno
Nantasenamat, Chanin
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Mahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, ThailandMahidol Univ, Ctr Data Min & Biomed Informat, Fac Med Technol, Bangkok 10700, Thailand
机构:Univ Bristol, Bristol Royal Infirm, Mol Neurobiol Unit, URCN Care Elderly, Bristol BS2 8HW, Avon, England
Tyler, SJ
Dawbarn, D
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机构:Univ Bristol, Bristol Royal Infirm, Mol Neurobiol Unit, URCN Care Elderly, Bristol BS2 8HW, Avon, England
Dawbarn, D
Wilcock, GK
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机构:Univ Bristol, Bristol Royal Infirm, Mol Neurobiol Unit, URCN Care Elderly, Bristol BS2 8HW, Avon, England
Wilcock, GK
Allen, SJ
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机构:
Univ Bristol, Bristol Royal Infirm, Mol Neurobiol Unit, URCN Care Elderly, Bristol BS2 8HW, Avon, EnglandUniv Bristol, Bristol Royal Infirm, Mol Neurobiol Unit, URCN Care Elderly, Bristol BS2 8HW, Avon, England