Damage control: cellular mechanisms of plasma membrane repair

Andrews, Norma W.; Almeida, Patrícia E. de; Corrotte, Matthias

doi:10.1016/j.tcb.2014.07.008

Cited by 260 publications

(269 citation statements)

References 74 publications

(136 reference statements)

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“…Live-cell imaging showed that complement exposure increased [Ca 2+ ] i and stimulated lysosome exocytosis. Lysosomal hydrolases and lipids released during exocytosis have been proposed to remodel the cell surface and limit membrane damage caused by pore-forming toxins (29). We show here that inactivating lysosomes causes sustained [Ca 2+ ] i elevation and mitochondrial fragmentation, indicating that lysosome exocytosis is a key mechanism for curtailing the downstream consequences of complement attack in the RPE.…”

Section: Discussionmentioning

confidence: 60%

“…In many cell types, elevated [Ca 2+ ] i has been shown to trigger fusion of lysosomes with the plasma membrane (25,28). Lysosome exocytosis, mediated by the lysosomal calcium sensor synaptotagmin 7 (Syt7), is vital for preserving membrane integrity after exposure to pore-forming toxins (29). We used live-cell imaging by total internal reflection fluorescence (TIRF) microscopy and complementary biochemical assays to determine whether sublytic MACs stimulate lysosome exocytosis in the RPE.…”

Section: Resultsmentioning

confidence: 99%

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Protective responses to sublytic complement in the retinal pigment epithelium

Tan

Toops

Lakkaraju

2016

Proc. Natl. Acad. Sci. U.S.A.

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The retinal pigment epithelium (RPE) is a key site of injury in inherited and age-related macular degenerations. Abnormal activation of the complement system is a feature of these blinding diseases, yet how the RPE combats complement attack is poorly understood. The complement cascade terminates in the cell-surface assembly of membrane attack complexes (MACs), which promote inflammation by causing aberrant signal transduction. Here, we investigated mechanisms crucial for limiting MAC assembly and preserving cellular integrity in the RPE and asked how these are compromised in models of macular degeneration. Using polarized primary RPE and the pigmented Abca4 −/− Stargardt disease mouse model, we provide evidence for two protective responses occurring within minutes of complement attack, which are essential for maintaining mitochondrial health in the RPE. First, accelerated recycling of the membrane-bound complement regulator CD59 to the RPE cell surface inhibits MAC formation. Second, fusion of lysosomes with the RPE plasma membrane immediately after complement attack limits sustained elevations in intracellular calcium and prevents mitochondrial injury. Cholesterol accumulation in the RPE, induced by vitamin A dimers or oxidized LDL, inhibits these defense mechanisms by activating acid sphingomyelinase (ASMase), which increases tubulin acetylation and derails organelle traffic. Defective CD59 recycling and lysosome exocytosis after complement attack lead to mitochondrial fragmentation and oxidative stress in the RPE. Drugs that stimulate cholesterol efflux or inhibit ASMase restore both these critical safeguards in the RPE and avert complement-induced mitochondrial injury in vitro and in Abca4 −/− mice, indicating that they could be effective therapeutic approaches for macular degenerations.he complement system is an important regulator of immunity and inflammation. Complement activation by the classical, alternative, or lectin pathways results in the assembly of C5b-9 membrane attack complexes (MACs), which form membrane pores and cause target cell lysis. Within the eye, a low level of constant complement activity is necessary for immune surveillance, and several membrane-bound and soluble regulators prevent excessive complement activation (1). An imbalance between complement activation and inhibition in the retina is implicated in the pathogenesis of age-related macular degeneration (AMD), which causes central vision loss in more than 30 million people globally (reviewed in refs. 2-4).Evidence suggests that the retinal pigment epithelium (RPE), which helps maintain ocular immune privilege, is the first line of defense against unregulated complement activation in the retina (5). The complement cascade is activated by insults that disturb RPE homeostasis, including defective clearance of phagocytosed photoreceptor outer segments (6) and abnormal accumulation of vitamin A dimers (7-9) or oxidized lipids (10) in the RPE. Studies also show that exposure to sublytic levels of MAC alters RPE barrier integrity, causes...

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Section: Discussionmentioning

confidence: 60%

Section: Resultsmentioning

confidence: 99%

Protective responses to sublytic complement in the retinal pigment epithelium

Tan

Toops

Lakkaraju

2016

Proc. Natl. Acad. Sci. U.S.A.

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“…In addition to improving our understanding of endothelial cell responses to membrane rupture, such as mitochondrial fission, tilted microindentation provides a highly versatile tool for studying membrane repair. Indeed, membrane repair processes are expected to differ depending on the size of the wound created in the membrane (55), which can be tuned by applying a controlled force with an indenter of controlled size. …”

Section: Discussionmentioning

confidence: 99%

Mechanical Criterion for the Rupture of a Cell Membrane under Compression

Gonzalez‐Rodriguez

Guillou

Cornat

et al. 2016

Biophysical Journal

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We investigate the mechanical conditions leading to the rupture of the plasma membrane of an endothelial cell subjected to a local, compressive force. Membrane rupture is induced by tilted microindentation, a technique used to perform mechanical measurements on adherent cells. In this technique, the applied force can be deduced from the measured horizontal displacement of a microindenter's tip, as imaged with an inverted microscope and without the need for optical sensors to measure the microindenter's deflection. We show that plasma membrane rupture of endothelial cells occurs at a well-defined value of the applied compressive stress. As a point of reference, we use numerical simulations to estimate the magnitude of the compressive stresses exerted on endothelial cells during the deployment of a stent.

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“…Several studies have reported that exocytosis of lysosomes contributes to the resealing of plasma membrane (Miyake and McNeil, 1995;Reddy et al, 2001;Chakrabarti et al, 2003;Andrews et al, 2014). By contrast, rapsyn has also been shown to interact with cytoskeletal proteins (Dobbins et al, 2008).…”

Section: Rapsyn Controls Lysosomal Exocytosismentioning

confidence: 99%

“…Increasing evidence suggests that lysosomal positioning plays an important role in coordinating cellular responses during nutrient starvation (Korolchuk et al, 2011). It has also been shown that lysosomal exocytosis plays an essential role in the resealing of the plasma membrane after damage (Miyake and McNeil, 1995;Reddy et al, 2001;Chakrabarti et al, 2003;Andrews et al, 2014). Here, we sought to examine whether rapsyn can be a key regulatory component of the dynamic state of lysosomes, notably lysosomal exocytosis.…”

Section: Introductionmentioning

confidence: 99%

Failure of lysosome clustering and positioning in the juxtanuclear region in cells deficient in rapsyn

Aittaleb

Chen

Akaaboune

2015

Journal of Cell Science

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Rapsyn, a scaffold protein, is required for the clustering of acetylcholine receptors (AChRs) at contacts between motor neurons and differentiating muscle cells. Rapsyn is also expressed in cells that do not express AChRs. However, its function in these cells remains unknown. Here, we show that rapsyn plays an AChRindependent role in organizing the distribution and mobility of lysosomes. In cells devoid of AChRs, rapsyn selectively induces the clustering of lysosomes at high density in the juxtanuclear region without affecting the distribution of other intracellular organelles. However, when the same cells overexpress AChRs, rapsyn is recruited away from lysosomes to colocalize with AChR clusters on the cell surface. In rapsyn-deficient (Rapsn −/− ) myoblasts or cells overexpressing rapsyn mutants, lysosomes are scattered within the cell and highly dynamic. The increased mobility of lysosomes in Rapsn −/− cells is associated with a significant increase in lysosomal exocytosis, as evidenced by increased release of lysosomal enzymes and plasma membrane damage when cells were challenged with the bacterial pore-forming toxin streptolysin-O. These findings uncover a new link between rapsyn, lysosome positioning, exocytosis and plasma membrane integrity.

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Damage control: cellular mechanisms of plasma membrane repair

Cited by 260 publications

References 74 publications

Protective responses to sublytic complement in the retinal pigment epithelium

Protective responses to sublytic complement in the retinal pigment epithelium

Mechanical Criterion for the Rupture of a Cell Membrane under Compression

Failure of lysosome clustering and positioning in the juxtanuclear region in cells deficient in rapsyn

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