What is pathophysiology of Alzheimer?

Yini i-pathophysiology ye-alzheimer?

I-Pathophysiology yesifo se-Alzheimer (AD) yindlela lehlangahlangene lefaka ekhatsi kuhlangana kwemaphrotheni langakavami, kuvuvuka, kanye nekungasebenti kahle kwemitsambo.

Timphawu letimbili letiyinhloko te-AD kuba khona kwe-amyloid-beta (Aβ) plaques kanye ne-neurofibrillary tangles (NFTs) ebuchosheni.

Ema-Amyloid-beta plaques akheka ngesikhatsi tincenye te amyloid precursor protein (APP) tijutjwa ngema-enzyme kute kwakheke ema-Aβ peptides.

Lama-peptide ahlangana bese akha ema-fibrilles langanyibiliki lahlangana ngaphandle kwemaseli ebuchopho, aphatamise kuchumana emkhatsini wemaseli futsi aholele ekufeni kwemaseli ebuchopho.

Kucina kwe-Aβ plaques kucatjangwa kutsi ngiko lokucala kucala i-AD, futsi kucatjangwa kutsi kunemtselela kulenchubo yekufa kwematsambo emtimba.

Ema-neurofibrillary tangles akheka ngesikhatsi i-protein tau iba ne-hyperphosphorylated bese yakha ema-filament langakavami ngekhatsi kwemaseli emtimba.

Letintfo letiyinkimbinkimbi tiphazamisa kusebenta kahle kwemashubhu lamancane, labalulekile ekutseni atfwele emanutrients kanye naletinye tintfo letidzingeka engcondvweni.

Lokugobana ekugcineni kubangela kutsi tinhlayiya letitsintsekile tife.

Kuvuvuka kwemtimba kuphindze kube nendzima ekwakhekeni kwe-AD.

Lamasotja emtimba aphendvula ekubutsaneni kwema-Aβ plaques nema-NFT ngekukhipha ema-cytokines lavikela kuvuvuka, lokungenta umonakalo kuma-neurons ube mubi kakhulu.

Ngetulu kwaloko, kunetinkhomba tekutsi kukhatsateka nge-oxidative, kungasebenti kahle kwemitokondri, kanye nekungasebenti kahle kwe-glucose metabolism kunemtselela ku-pathophysiology ye-AD.

Letintfo tingabangela kutsi tinhlayiya tingaphili kahle futsi tife, lokwenta kugula kuchubeke.

Ngalokuvamile, i-AD ihlanganisa tintfo letinyenti letibangela kutsi umuntfu angakhoni kucabanga kahle futsi akhumbule tintfo letinyenti.

['Tintfo letibhalwe phansi']

PubMed/Medline https://www.nlm.nih.gov/databases/download/pubmed_medline.html

RefinedWeb https://arxiv.org/abs/2306.01116

Nemeroff CB: The preeminent role of neuropeptide systems in the early pathophysiology of Alzheimer disease: up with corticotropin-releasing factor, down with acetylcholine. Arch Gen Psychiatry. 1999, 56 (11): 991-2.

Skoog I, Kalaria RN, Breteler MM: Vascular factors and Alzheimer disease. Alzheimer Dis Assoc Disord. , 13 Suppl 3 (): S106-14.

Proft J, Weiss N: Jekyll and Hide: The two faces of amyloid β. Commun Integr Biol. 2012, 5 (5): 405-7.

Whitehouse PJ, Hedreen JC, White CL, Price DL: Basal forebrain neurons in the dementia of Parkinson disease. Ann Neurol. 1983, 13 (3): 243-8.

Casadesus G, Moreira PI, Nunomura A, Siedlak SL, Bligh-Glover W, Balraj E, Petot G, Smith MA, Perry G: Indices of metabolic dysfunction and oxidative stress. Neurochem Res. , 32 (4-5): 717-22.

Candore G, Bulati M, Caruso C, Castiglia L, Colonna-Romano G, Di Bona D, Duro G, Lio D, Matranga D, Pellicanò M, Rizzo C, Scapagnini G, Vasto S: Inflammation, cytokines, immune response, apolipoprotein E, cholesterol, and oxidative stress in Alzheimer disease: therapeutic implications. Rejuvenation Res. , 13 (2-3): 301-13.

Raskind MA, Peskind ER: Neurobiologic bases of noncognitive behavioral problems in Alzheimer disease. Alzheimer Dis Assoc Disord. 1994, 8 Suppl 3 (): 54-60.

Schindler SE, McConathy J, Ances BM, Diamond MI: Advances in diagnostic testing for Alzheimer disease. Mo Med. , 110 (5): 401-5.

Singh VK: Immune-activation model in Alzheimer disease. Mol Chem Neuropathol. , 28 (1-3): 105-11.

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What is pathophysiology of alzheimer?

The pathophysiology of Alzheimer's disease (AD) is a complex process that involves the accumulation of abnormal proteins, inflammation, and neuronal dysfunction.

The two main hallmarks of AD are the presence of amyloid-beta (Aβ) plaques and neurofibrillary tangles (NFTs) in the brain.

Amyloid-beta plaques are formed when fragments of the amyloid precursor protein (APP) are cleaved by enzymes to form Aβ peptides.

These peptides aggregate and form insoluble fibrils that accumulate outside neurons, disrupting cell-to-cell communication and leading to neuronal death.

The accumulation of Aβ plaques is thought to be one of the earliest events in the development of AD, and it is believed to contribute to the neurodegenerative process.

Neurofibrillary tangles are formed when the protein tau becomes hyperphosphorylated and forms abnormal filaments inside neurons.

These tangles disrupt the normal functioning of the microtubules, which are essential for the transport of nutrients and other materials within the neuron.

The tangles eventually lead to the death of the affected neurons.

Inflammation also plays a role in the pathophysiology of AD.

The immune system responds to the accumulation of Aβ plaques and NFTs by releasing pro-inflammatory cytokines, which can exacerbate the damage to neurons.

Additionally, there is evidence that oxidative stress, mitochondrial dysfunction, and impaired glucose metabolism contribute to the pathophysiology of AD.

These factors can lead to neuronal dysfunction and death, further exacerbating the disease process.

Overall, the pathophysiology of AD is a complex interplay of multiple factors that ultimately lead to the progressive decline in cognitive function and memory loss that characterizes the disease.

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