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Dive into the research topics where Lisa Mcconlogue is active.

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Featured researches published by Lisa Mcconlogue.


Journal of Biological Chemistry | 2001

Retention of the Alzheimer's Amyloid Precursor Fragment C99 in the Endoplasmic Reticulum Prevents Formation of Amyloid β-Peptide

William A. Maltese; Susan E. Wilson; Yizheng Tan; Susanna Suomensaari; Sukanto Sinha; Robin Barbour; Lisa Mcconlogue

γ-Secretase is a membrane-associated endoprotease that catalyzes the final step in the processing of Alzheimers β-amyloid precursor protein (APP), resulting in the release of amyloid β-peptide (Aβ). The molecular identity of γ-secretase remains in question, although recent studies have implicated the presenilins, which are membrane-spanning proteins localized predominantly in the endoplasmic reticulum (ER). Based on these observations, we have tested the hypothesis that γ-secretase cleavage of the membrane-anchored C-terminal stump of APP (i.e. C99) occurs in the ER compartment. When recombinant C99 was expressed in 293 cells, it was localized mainly in the Golgi apparatus and gave rise to abundant amounts of Aβ. Co-expression of C99 with mutant forms of presenilin-1 (PS1) found in familial Alzheimers disease resulted in a characteristic elevation of the Aβ42/Aβ40 ratio, indicating that the N-terminal exodomain of APP is not required for mutant PS1 to influence the site of γ-secretase cleavage. Biogenesis of both Aβ40 and Aβ42 was almost completely eliminated when C99 was prevented from leaving the ER by addition of a di-lysine retention motif (KKQN) or by co-expression with a dominant-negative mutant of the Rab1B GTPase. These findings indicate that the ER is not a major intracellular site for γ-secretase cleavage of C99. Thus, by inference, PS1 localized in this compartment does not appear to be active as γ-secretase. The results suggest that presenilins may acquire the characteristics of γ-secretase after leaving the ER, possibly by assembling with other proteins in peripheral membranes.


Archive | 1994

Methods of screening for β-amyloid peptide production inhibitors

Lisa Mcconlogue; Dale Schenk; Peter Seubert; Sukanto Sinha; Jun Zhao


Archive | 2005

β-secretase enzyme compositions and methods

John P. Anderson; Guriqbal S. Basi; Minh Tam Doan; Normand Frigon; Varghese John; Michael Power; Sukanto Sinha; Gwen Tatsuno; Jay Tung; Shuwen Wang; Lisa Mcconlogue


Archive | 1996

Method for identifying alzheimer's disease therapeutics using transgenic animal models

Lisa Mcconlogue; Peter Seubert


Archive | 1996

Beta-secretase, antibodies to beta-secretase, and assays for detecting beta-secretase inhibition

John P. Anderson; Susanna M. S. Chrysler; Kirsten L. Jacobson-Croak; Pamela S. Keim; Lisa Mcconlogue; Sukanto Sinha; Hua Tan


Archive | 1998

Method for selecting a transgenic mouse model of alzheimer's disease

Kate Dora Games; Dale Schenk; Lisa Mcconlogue; Peter Seubert; Russell E. Rydel


Archive | 2001

Selecting compounds to reduce inflammation associated with Alzheimer's disease

Lisa Mcconlogue; Kate Dora Games; Theodore Yednock; Tan Hua; Elizabeth Messersmith; Frederique Bard


Archive | 2003

Testing compounds for effects on synaptophysin in transgenic mice expressing an Alzheimer's disease FAD DNA sequence

Kate Dora Games; Dale Schenk; Lisa Mcconlogue; Peter Seubert; Russell E. Rydel


Archive | 2000

b-secretase inhibitor

John P. Anderson; Guriqbal S. Basi; Minh Tam Doane; Normand Frigon; Varghese John; Michael Power; Sukanto Sinha; Gwen Tatsuno; Jay Tung; Shuwen Wang; Lisa Mcconlogue


Archive | 2001

Screening markers and methods for neurodegenerative disorders

Lisa Mcconlogue; Elizabeth Messersmith; Frederique Bard

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Sukanto Sinha

University of California

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Varghese John

Buck Institute for Research on Aging

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Jay S. Tung

Thomas Jefferson University

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Robin Barbour

University of Toledo Medical Center

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Susan E. Wilson

University of Toledo Medical Center

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