Tau-Centric Targets and Drugs in Clinical Development for the Treatment of Alzheimer’s Disease

Panza, Francesco; Solfrizzi, Vincenzo; Seripa, Davide; Imbimbo, Bruno P.; Lozupone, Madia; Santamato, Andrea; Zecca, Chiara; Barulli, Maria Rosaria; Bellomo, Antonello; Pilotto, Alberto; Daniele, Antonio; Greco, Antonio; Logroscino, Giancarlo

doi:10.1155/2016/3245935

Cited by 157 publications

(110 citation statements)

References 157 publications

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“…net) fos fo rili ni mas [37]. Ly gi nant to kio pa ties am þiaus svei kø ir sergan èiø AL as me nø tau bal ty mo kie ká sme ge ny se, nu sta tyta, kad ser gan èiø jø sme ge ny se tau yra 4-5 kar tus dau giau, o ðis skir tu mas su si da ro dël hi per fos fo ri lin to tau [41]. Hiper fos fo ri lin to tau mo liui pri klau so 3-4 kar tus dau giau fos fa to mo liø, ne gu fi zio lo gið kai fos fo ri lin tam bal ty mui [39].…”

Section: Tau Baltymas Alzheimerio Ligos Patogenezëjeunclassified

“…Ma þë ja hi per fos fo ri lin to tau afi nið ku mas mik ro tu bulëms, jis at si ski ria, to dël dau gë ja in tra ci top laz mi nio tau kie kis [37]. Ci top laz mo je su si da ro tau oli go me rai -nuo dime rø iki ok ta me rø, for muo jan tys ne tir pius fi la men tus, ið ku riø su si da ro neu ro fib ri li niø tin kle liø ðer dis [41]. Dau gë -jant tau, jis stip riau sà vei kau ja su ki tais làs te lës bal ty mais, truk do at lik ti jiems ápras tas funk ci jas, taip pat "ið stu mia" juos ið ápras tø lo ka li za ci jø neu ro nuo se, ka dan gi hi per fosfo ri lin tas tau uþ pil do neu ro no kû nà ir den dri tus [37,39].…”

Section: Tau Baltymas Alzheimerio Ligos Patogenezëjeunclassified

“…Dau gë -jant tau, jis stip riau sà vei kau ja su ki tais làs te lës bal ty mais, truk do at lik ti jiems ápras tas funk ci jas, taip pat "ið stu mia" juos ið ápras tø lo ka li za ci jø neu ro nuo se, ka dan gi hi per fosfo ri lin tas tau uþ pil do neu ro no kû nà ir den dri tus [37,39]. Be to, ma þë ja si nap siø skai èius [41]. Pro gre suo jant li gai, tau ima sà vei kau ti su re ak ty viais kar bo nilo jun gi niais, dël to su si for muo ja su dë tin ges ni gli kuo ti ga lu ti niai pro duk tai, at spa rûs pro te o li zei, tai gi dar la biau ska ti na ma ag re ga ci ja [39].…”

Section: Tau Baltymas Alzheimerio Ligos Patogenezëjeunclassified

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Alzheimerio ligos gydymo metodų paieška: klinikinių tyrimų kryptys

Pakulaitė

Regelskytė

Audronytė

et al. 2018

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Vilniaus universiteto Medicinos fakulteto Klinikinës medicinos instituto Neurologijos ir neurochirurgijos klinika ÁVADASAlz hei me rio li ga (AL) -lë ti në pro gre suo jan ti, ne gráþ ta mø po ky èiø sme ge ny se su ke lian ti li ga [1]. Tai daþ niau sia demen ci jos prie þas tis, su da ran ti 60-70 % vi sø de men ci jø, o jos pa pli ti mas itin di dë ja il gë jant gy ve ni mo truk mei [2,3]. AL su ke lia di de lae eko no mi nae nað tà, taip pat tam pa vis daþ -nes ne mir ties prie þas ti mi [3]. Stu di jø duo me ni mis, mir tingu mas nuo in sul to ir ðir dies li gø ma þë ja, ta èiau AL, kaip mir ties prie þas tis tarp vy res niø nei 75 me tø am þiaus pa cientø, mi n i ma jau ne ðeð to je, o tre èio je vie to je pa gal daþ ná po kar dio vas ku li niø ir ce reb ro vas ku li niø li gø bei vë þio [3,4]. AL gy dy mo kli ni ki niø ty ri mø pra dþia lai ko mi 1980-1990 m., kai pra dë ti nau do ti cho li nes te ra zës in hi bito riai [5]. 1974 m. Drach man ir Le a vitt su sie jo cen tri niø cho li ner gi niø neu ro nø pa þei di mà su at min ties blo gë ji mu ir am þiu mi, o vë les në se stu di jo se Da vis ir Ma lo ney ap ra ðë cho li ner gi nio Mei ner to bran duo lio (angl. nu cleus basalis of Meynert) pa þei di mà pa cien tams, ser gan tiems AL [6,7]. Ma ny ta, kad cho li ner gi nës sis te mos pa þei di mas, ser gant AL, pa na ðus á do pa mi ner gi nës sis te mos pa þei di mà, sergant Par kin so no li ga [8]. Pir mà já cho li nes te ra zës in hi bi toriø tak ri nà leng vai ir vi du ti nio sun ku mo Alz hei me rio ti po de men ci jai gy dy ti 1993 m. áre gist ra vo JAV Mais to ir vaistø ad mi nist ra ci ja (angl. Food and Drug Ad min is tra tion, FDA), ta èiau jis ne be nau do ja mas dël ne pa gei dau ja mø reið ki niø (virð ki na mo jo trak to simp to mø) ir ma þo efek tyvu mo [9,10]. Nuo to lai ko bu vo at lik ta ir ðiuo me tu vyks ta dau gy bë kli ni ki niø ty ri mø, ta èiau tik 3 cho li nes te ra zës inhi bi to riai (do ne pe zi lis, ri vas tig mi nas (jo pe ro ra li në ir trans der ma li në for mos), ga lan ta mi nas) ir glu ta ma ter gi nae sis te mà vei kian tis me man ti nas ty ri muo se pa ro dë pa kan kamà efek ty vu mà bei sau gu mà ir bu vo áre gist ruo ti gy dy ti AL [10]. Ðie vais tai, skir ti simp to mi niam AL gy dy mui, ðiek tiek pa leng vi na li gos kli ni ki nae ið raið kà, ta èiau jø efek ty vumas në ra di de lis, jie ne vei kia li gos prie þas ties ir ne su stabdo li gos pro gre sa vi mo [10,11]. Pas ku ti nis vais tas AL gydy ti -me man ti nas -Eu ro po je bu vo áre gist ruo tas 2002 m., o JAV -2003 m. [10]. Vais tø, skir tø AL gy dy ti, kli ni ki niai ty ri mai vyks ta jau ke lis de ðimt me èius, ta èiau 15 me tø neran da ma nau jø efek ty viø ir sau giø vais tø.Pas ta rà já de ðimt me tá dau giau sia kli ni ki niø ty ri mø at lieka ma su vais tais, po ten cia liai ga lin èiais mo di fi kuo ti AL ei - Adresas: Gy të Pa ku lai të Vil niaus uni ver si te to li go ni nës San ta ros kli ni kos, Neurologijos cen tras San ta rið kiø g. 2, LT-08661 Vil nius El. pa ðtas gyte.pakulaite@gmail.comSan tra...

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Section: Tau Baltymas Alzheimerio Ligos Patogenezëjeunclassified

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Alzheimerio ligos gydymo metodų paieška: klinikinių tyrimų kryptys

Pakulaitė

Regelskytė

Audronytė

et al. 2018

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show abstract

“…In the last decade, different classes of tau aggregation inhibitors (TAIs) have been reported, including polyphenols [31], porphyrins [32], phenothiazines such as Methylene blue [32], benzothiazoles/cyanines such as N744 and Riluzole [33], thioxothiazolidinones (rhodanines), phenylthiazolehydrazides, anthraquinones, and aminothienopyridazines (ATPZs) [30,33] (Table 2).…”

Section: Tau Aggregation Inhibitormentioning

confidence: 99%

Inhibitors of protein aggregates as novel drugs in neurodegenerative diseases

Pietrobono¹,

Giacomelli²,

Ml³

et al. 2017

Glob Drugs Therap

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“…Because of this, preventing tau acetylation is critical for stopping disease onset. Salsalate and methylene blue have both been shown to reduce tau acetylation in pre-clinical models, however the exact mechanism has not been fully elucidated and warrants further investigation [10]. It is likely that these drugs are limiting the expansion of secondary injury cascades following insult.…”

Section: Introductionmentioning

confidence: 99%

Role of Tau Acetylation in Alzheimer’s Disease and Chronic Traumatic Encephalopathy: The Way Forward for Successful Treatment

et al. 2017

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Progressive neurodegenerative diseases plague millions of individuals both in the United States and across the world. The current pathology of progressive neurodegenerative tauopathies, such as Alzheimer's disease (AD), Pick's disease, frontotemporal dementia (FTD), and progressive supranuclear palsy, primarily revolves around phosphorylation and hyperphosphorylation of the tau protein. However, more recent evidence suggests acetylation of tau protein at lysine 280 may be a critical step in molecular pathology of these neurodegenerative diseases prior to the tau hyperphosphorylation. Secondary injury cascades such as oxidative stress, endoplasmic reticulum stress, and neuroinflammation contribute to lasting damage within the brain and can be induced by a number of different risk factors. These injury cascades funnel into a common pathway of early tau acetylation, which may serve as the catalyst for progressive degeneration. The post translational modification of tau can result in production of toxic oligomers, contributing to reduced solubility as well as aggregation and formation of neurofibrillary tangles, the hallmark of AD pathology. Chronic Traumatic Encephalopathy (CTE), caused by repetitive brain trauma is also associated with a hyperphosphorylation of tau. We postulated acetylation of tau at lysine 280 in CTE disease could be present prior to the hyperphosphorylation and tested this hypothesis in CTE pathologic specimens. We also tested for ac-tau 280 in early stage Alzheimer's disease (Braak stage 1). Histopathological examination using the ac tau 280 antibody was performed in three Alzheimer's cases and three CTE patients. Presence of ac-tau 280 was confirmed in all cases at early sites of disease manifestation. These findings suggest that tau acetylation may precede tau phosphorylation and could be the first "triggering" event leading to neuronal loss. To the best of our knowledge, this is the first study to identify acetylation of the tau protein in CTE. Prevention of tau acetylation could possibly serve as a novel target for stopping neurodegeneration before it fully begins. In this study, we highlight what is known about tau acetylation and neurodegeneration.

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Tau-Centric Targets and Drugs in Clinical Development for the Treatment of Alzheimer’s Disease

Cited by 157 publications

References 157 publications

Alzheimerio ligos gydymo metodų paieška: klinikinių tyrimų kryptys

Alzheimerio ligos gydymo metodų paieška: klinikinių tyrimų kryptys

Inhibitors of protein aggregates as novel drugs in neurodegenerative diseases

Role of Tau Acetylation in Alzheimer’s Disease and Chronic Traumatic Encephalopathy: The Way Forward for Successful Treatment

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