Presenilins Are Enriched in Endoplasmic Reticulum Membranes Associated with Mitochondria

Area‐Gómez, Estela; Groof, A.J.C. de; Boldogh, István; Bird, Thomas D.; Gibson, Gary E.; Koehler, Carla M.; Yu, Wen H.; Duff, Karen; Yaffe, Michael P.; Pon, Liza A.; Schon, Eric A.

doi:10.2353/ajpath.2009.090219

Cited by 350 publications

(337 citation statements)

References 54 publications

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“…In previous reports, we showed that γ‐secretase activity is localized in MAM (Area‐Gomez et al , 2009) and that alterations in γ‐secretase activity result in the upregulation of MAM function and in increased ER–mitochondria apposition (Area‐Gomez et al , 2012). We now show that the γ‐secretase substrate C99, in addition to its endosomal localization, is also present in MAM domains.…”

Section: Discussionmentioning

confidence: 80%

“…Consistent with the data of others (Das et al , 2016), FL‐APP and BACE1 co‐migrated partially with a marker for endosomes (Rab7), but not with lysosomal, ER‐intermediate, or MAM markers (Fig 2C). Similarly, the APP‐CTFs C83 and C99 co‐migrated with endosomal and lysosomal markers (Rab5, Rab7, and LAMP‐2) (Haass et al , 2012; Das et al , 2016), whereas PS1 co‐migrated with MAM markers, such as FACL4 (Area‐Gomez et al , 2009; Newman et al , 2014; Schreiner et al , 2015). We reasoned that the difficulty in seeing APP‐CTFs and PS1 together was probably due to the rapid cleavage of the CTFs by γ‐secretase once both are in the same compartment.…”

Section: Resultsmentioning

confidence: 99%

“…We and others have shown that presenilins and γ‐secretase activity localize to MAM (Area‐Gomez et al , 2009; Newman et al , 2014; Schreiner et al , 2015). Moreover, MAM functionality (Area‐Gomez et al , 2012) and ER–mitochondrial apposition (Area‐Gomez et al , 2012; Hedskog et al , 2013) are increased in AD.…”

Section: Introductionmentioning

confidence: 83%

“…We propose that, while the majority of C99 resides in endosomes, C99 can traffic to MAM regions in the ER, where it is cleaved rapidly by γ‐secretase to produce Aβ and AICD (Area‐Gomez et al , 2009; Schreiner et al , 2015). We note that although the mechanism by which C99 translocates to ER‐MAM is unknown, recent work has demonstrated the existence of ER‐endosome contacts (Rowland et al , 2014) where lipid and protein exchange may occur (Wilhelm et al , 2017).…”

Section: Discussionmentioning

confidence: 99%

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Increased localization of APP‐C99 in mitochondria‐associated ER membranes causes mitochondrial dysfunction in Alzheimer disease

et al. 2017

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In the amyloidogenic pathway associated with Alzheimer disease (AD), the amyloid precursor protein (APP) is cleaved by β‐secretase to generate a 99‐aa C‐terminal fragment (C99) that is then cleaved by γ‐secretase to generate the β‐amyloid (Aβ) found in senile plaques. In previous reports, we and others have shown that γ‐secretase activity is enriched in mitochondria‐associated endoplasmic reticulum (ER) membranes (MAM) and that ER–mitochondrial connectivity and MAM function are upregulated in AD. We now show that C99, in addition to its localization in endosomes, can also be found in MAM, where it is normally processed rapidly by γ‐secretase. In cell models of AD, however, the concentration of unprocessed C99 increases in MAM regions, resulting in elevated sphingolipid turnover and an altered lipid composition of both MAM and mitochondrial membranes. In turn, this change in mitochondrial membrane composition interferes with the proper assembly and activity of mitochondrial respiratory supercomplexes, thereby likely contributing to the bioenergetic defects characteristic of AD.

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Section: Discussionmentioning

confidence: 80%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 83%

Section: Discussionmentioning

confidence: 99%

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Increased localization of APP‐C99 in mitochondria‐associated ER membranes causes mitochondrial dysfunction in Alzheimer disease

et al. 2017

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“…We reported previously that PS1, PS2, and γ‐secretase activities are highly enriched in the MAM 10 and that ER–mitochondrial communication and MAM function, including phospholipid and cholesteryl ester synthesis, are increased dramatically in presenilin‐mutant and presenilin‐deficient cells and in cells from AD patients 7. Both lines of evidence support the view that PS1 and PS2, in addition to generating Aβ, are negative regulators of MAM function 7 and that these alterations play a critical role in the pathogenesis of the disease (the “MAM hypothesis”) 11, 12.…”

Section: Resultsmentioning

confidence: 92%

ApoE4 upregulates the activity of mitochondria‐associated ER membranes

et al. 2015

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In addition to the appearance of senile plaques and neurofibrillary tangles, Alzheimer's disease (AD) is characterized by aberrant lipid metabolism and early mitochondrial dysfunction. We recently showed that there was increased functionality of mitochondria‐associated endoplasmic reticulum (ER) membranes (MAM), a subdomain of the ER involved in lipid and cholesterol homeostasis, in presenilin‐deficient cells and in fibroblasts from familial and sporadic AD patients. Individuals carrying the ε4 allele of apolipoprotein E (ApoE4) are at increased risk for developing AD compared to those carrying ApoE3. While the reason for this increased risk is unknown, we hypothesized that it might be associated with elevated MAM function. Using an astrocyte‐conditioned media (ACM) model, we now show that ER–mitochondrial communication and MAM function—as measured by the synthesis of phospholipids and of cholesteryl esters, respectively—are increased significantly in cells treated with ApoE4‐containing ACM as compared to those treated with ApoE3‐containing ACM. Notably, this effect was seen with lipoprotein‐enriched preparations, but not with lipid‐free ApoE protein. These data are consistent with a role of upregulated MAM function in the pathogenesis of AD and may help explain, in part, the contribution of ApoE4 as a risk factor in the disease.

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Emerging functions of the mitochondria–ER–lipid droplet three‐way junction in coordinating lipid transfer, metabolism, and storage in cells

Monteiro‐Cardoso,

Giordano

2024

FEBS Letters

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Over the past two decades, we have witnessed a growing appreciation for the importance of membrane contact sites (CS) in facilitating direct communication between organelles. CS are tiny regions where the membranes of two organelles meet but do not fuse and allow the transfer of metabolites between organelles, playing crucial roles in the coordination of cellular metabolic activities. The significant advancements in imaging techniques and molecular and cell biology research have revealed that CS are more complex than what originally thought, and as they are extremely dynamic, they can remodel their shape, composition, and functions in accordance with metabolic and environmental changes and can occur between more than two organelles. Here, we describe how recent studies led to the identification of a three‐way mitochondria–ER–lipid droplet CS and discuss the emerging functions of these contacts in maintaining lipid storage, homeostasis, and balance. We also summarize the properties and functions of key protein components localized at the mitochondria–ER–lipid droplet interface, with a special focus on lipid transfer proteins. Understanding tripartite CS is essential for unraveling the complexities of inter‐organelle communication and cooperation within cells.

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Presenilins Are Enriched in Endoplasmic Reticulum Membranes Associated with Mitochondria

Cited by 350 publications

References 54 publications

Increased localization of APP‐C99 in mitochondria‐associated ER membranes causes mitochondrial dysfunction in Alzheimer disease

Increased localization of APP‐C99 in mitochondria‐associated ER membranes causes mitochondrial dysfunction in Alzheimer disease

ApoE4 upregulates the activity of mitochondria‐associated ER membranes

Emerging functions of the mitochondria–ER–lipid droplet three‐way junction in coordinating lipid transfer, metabolism, and storage in cells

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