Efficient inhibition of the Alzheimer's disease β-secretase by membrane targeting

Lawrence Rajendran; Anja Schneider; Georg Schlechtingen; Sebastian Weidlich; Jonas Ries; Tobias Braxmeier; Petra Schwille; Jörg B. Schulz; Cornelia Schroeder; Mikael Simons; Gary Jennings; Hans Joachim Knölker; Kai Simons

doi:10.1126/science.1156609

Efficient inhibition of the Alzheimer's disease β-secretase by membrane targeting

Lawrence Rajendran
, Anja Schneider
, Georg Schlechtingen
, Sebastian Weidlich
, Jonas Ries
, Tobias Braxmeier
, Petra Schwille
, Jörg B. Schulz
, Cornelia Schroeder
, Mikael Simons
, Gary Jennings
, Hans Joachim Knölker
, Kai Simons

Publikation: Beitrag in Fachzeitschrift › Artikel › Begutachtung

232 Zitate (Scopus)

Abstract

β-Secretase plays a critical role in β-amyloid formation and thus provides a therapeutic target for Alzheimer's disease. Inhibitor design has usually focused on active-site binding, neglecting the subcellular localization of active enzyme. We have addressed this issue by synthesizing a membrane-anchored version of a β-secretase transition-state inhibitor by linking it to a sterol moiety. Thus, we targeted the inhibitor to active β-secretase found in endosomes and also reduced the dimensionality of the inhibitor, increasing its local membrane concentration. This inhibitor reduced enzyme activity much more efficiently than did the free inhibitor in cultured cells and in vivo. In addition to effectively targeting β-secretase, this strategy could also be used in designing potent drugs against other membrane protein targets.

Originalsprache	Englisch
Seiten (von - bis)	520-523
Seitenumfang	4
Fachzeitschrift	Science
Jahrgang	320
Ausgabenummer	5875
DOIs	https://doi.org/10.1126/science.1156609
Publikationsstatus	Veröffentlicht - 25 Apr. 2008
Extern publiziert	Ja

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title = "Efficient inhibition of the Alzheimer's disease β-secretase by membrane targeting",

abstract = "β-Secretase plays a critical role in β-amyloid formation and thus provides a therapeutic target for Alzheimer's disease. Inhibitor design has usually focused on active-site binding, neglecting the subcellular localization of active enzyme. We have addressed this issue by synthesizing a membrane-anchored version of a β-secretase transition-state inhibitor by linking it to a sterol moiety. Thus, we targeted the inhibitor to active β-secretase found in endosomes and also reduced the dimensionality of the inhibitor, increasing its local membrane concentration. This inhibitor reduced enzyme activity much more efficiently than did the free inhibitor in cultured cells and in vivo. In addition to effectively targeting β-secretase, this strategy could also be used in designing potent drugs against other membrane protein targets.",

author = "Lawrence Rajendran and Anja Schneider and Georg Schlechtingen and Sebastian Weidlich and Jonas Ries and Tobias Braxmeier and Petra Schwille and Schulz, \{J{\"o}rg B.\} and Cornelia Schroeder and Mikael Simons and Gary Jennings and Kn{\"o}lker, \{Hans Joachim\} and Kai Simons",

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doi = "10.1126/science.1156609",

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T1 - Efficient inhibition of the Alzheimer's disease β-secretase by membrane targeting

AU - Rajendran, Lawrence

AU - Schneider, Anja

AU - Schlechtingen, Georg

AU - Weidlich, Sebastian

AU - Ries, Jonas

AU - Braxmeier, Tobias

AU - Schwille, Petra

AU - Schulz, Jörg B.

AU - Schroeder, Cornelia

AU - Simons, Mikael

AU - Jennings, Gary

AU - Knölker, Hans Joachim

AU - Simons, Kai

PY - 2008/4/25

Y1 - 2008/4/25

N2 - β-Secretase plays a critical role in β-amyloid formation and thus provides a therapeutic target for Alzheimer's disease. Inhibitor design has usually focused on active-site binding, neglecting the subcellular localization of active enzyme. We have addressed this issue by synthesizing a membrane-anchored version of a β-secretase transition-state inhibitor by linking it to a sterol moiety. Thus, we targeted the inhibitor to active β-secretase found in endosomes and also reduced the dimensionality of the inhibitor, increasing its local membrane concentration. This inhibitor reduced enzyme activity much more efficiently than did the free inhibitor in cultured cells and in vivo. In addition to effectively targeting β-secretase, this strategy could also be used in designing potent drugs against other membrane protein targets.

AB - β-Secretase plays a critical role in β-amyloid formation and thus provides a therapeutic target for Alzheimer's disease. Inhibitor design has usually focused on active-site binding, neglecting the subcellular localization of active enzyme. We have addressed this issue by synthesizing a membrane-anchored version of a β-secretase transition-state inhibitor by linking it to a sterol moiety. Thus, we targeted the inhibitor to active β-secretase found in endosomes and also reduced the dimensionality of the inhibitor, increasing its local membrane concentration. This inhibitor reduced enzyme activity much more efficiently than did the free inhibitor in cultured cells and in vivo. In addition to effectively targeting β-secretase, this strategy could also be used in designing potent drugs against other membrane protein targets.

UR - https://www.scopus.com/pages/publications/42549148456

U2 - 10.1126/science.1156609

DO - 10.1126/science.1156609

M3 - Article

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AN - SCOPUS:42549148456

SN - 0036-8075

VL - 320

SP - 520

EP - 523

JO - Science

JF - Science

IS - 5875

ER -

Efficient inhibition of the Alzheimer's disease β-secretase by membrane targeting

Abstract

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