Phosphatidylserine exposure during apoptosis reflects bidirectional trafficking between plasma membrane and cytoplasm

Sh, Lee; Meng, XW; Ks, Flatten; Da, Loegering; Kaufmann, Scott H.

doi:10.1038/cdd.2012.93

Cited by 173 publications

(142 citation statements)

References 42 publications

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“…We assume that autophagic vesicles expelled by maturing reticulocytes would be phagocytosed in vivo by splenic macrophages in individuals with a functional spleen. Our data suggests that a bidirectional trafficking process, as proposed by Lee et al, 8 is used to generate erythrocytes from mature reticulocytes. However, in the maturing human reticulocyte, this apoptotic-like process combines with autophagy to achieve the reduction in surface area and volume, and simultaneously eliminate unwanted residual intracellular organelles in order to form the biconcave erythrocyte.…”

supporting

confidence: 60%

Autophagic vesicles on mature human reticulocytes explain phosphatidylserine-positive red cells in sickle cell disease

Mankelow

Griffiths

Trompeter

et al. 2015

Blood

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Key Points• Reticulocyte maturation involves the release of intact, inside-out autophagic vesicles with PS exposed on their surface.• Elevated levels of autophagic vesicles on circulating reticulocytes cause PS exposure in patients with SCD.During maturation to an erythrocyte, a reticulocyte must eliminate any residual organelles and reduce its surface area and volume. Here we show this involves a novel process whereby large, intact, inside-out phosphatidylserine (PS)-exposed autophagic vesicles are extruded. Cell surface PS is a well-characterized apoptotic signal initiating phagocytosis. In peripheral blood from patients after splenectomy or in patients with sickle cell disease (SCD), the number of circulating red cells exposing PS on their surface is elevated. We show that in these patients PS is present on the cell surface of red cells in large (∼1.4 mm) discrete areas corresponding to autophagic vesicles. The autophagic vesicles found on reticulocytes are identical to those observed on red cells from splenectomized individuals and patients with SCD. Our data suggest the increased thrombotic risk associated with splenectomy, and patients with hemoglobinopathies is a possible consequence of increased levels of circulating mature reticulocytes expressing inside-out PS-exposed autophagic vesicles because of asplenia. (Blood. 2015;126(15):1831-1834) IntroductionThe erythrocyte is one of the most abundant, accessible, and best characterized of human cells but until the recent development of in vitro erythroid culture systems 1,2 obtaining large numbers of its precursor cell, the human reticulocyte has been problematic. Reticulocytes are broadly grouped into R1, motile multilobular, and normally confined to bone marrow, and R2, which are nonmotile, much more mechanically stable, and released into peripheral circulation where they comprise ;2% of red blood cells.3,4 During maturation to an erythrocyte, the reticulocyte must lose ;20% of its surface area, reduce its volume, and degrade or eliminate residual cytosolic organelles. Current dogma considers that loss of plasma membrane is through the release of endocytosed plasma membrane as exosomes, whereas purging of cellular organelles is executed by autophagy. 5Surface phosphatidylserine (PS) exposure is a well characterized signal for initiating phagocytosis of unwanted cells or cellular material. 6PS is normally located on the intracellular surface of plasma membranes. Relocation to the extracellular surface may occur by activation of a scramblase 7 or a bidirectional trafficking process involving cytosolic vesicles.8 PS-exposed red cells are found in the peripheral blood of patients who have undergone splenectomy, or have sickle cell disease (SCD) or thalassemia. 9-13 Study designFor details of anonymized patient samples, antibodies used, and full methods, see supplemental Methods, available on the Blood Web site. Briefly, reticulocytes were derived from erythroid cultures and confocal microscopy was performed as described.2 PS was detected using Annexin V fluore...

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supporting

confidence: 60%

Autophagic vesicles on mature human reticulocytes explain phosphatidylserine-positive red cells in sickle cell disease

Mankelow

Griffiths

Trompeter

et al. 2015

Blood

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“…Consistent with these data, apoptosis was also evident from western blots that revealed cleavage of wellestablished caspase substrates 30 such as poly(ADP-ribose) polymerase 1 (PARP1) and procaspase-3 (Figure 1c), as well as flow cytometry showing increased annexin V staining (see below), another hallmark of apoptosis. 31 Although previously noted, 5 formation of reactive oxygen species (ROS) was not observed in any of the three AML lines treated with MLN4924 (Supplementary Figure S1c), whereas increased ROS were readily detected upon exposure to the positive control adaphostin, an agent that inhibits mitochondrial electron transport to induce ROS. 32 Evidence of endoplasmic reticulum (ER) stress also was not present, as levels of ATF4, GRP78, and phospho-EIF2α remained unchanged in response to MLN4924 treatment (Supplementary Figure S1d).…”

Section: Mln4924mentioning

confidence: 82%

“…Cells were exposed to increasing concentrations of MLN4924 diluted in DMSO (final concentration 0.1% v/v) for 4-48 h, then pelleted and stained with PI as previously described. 29,31 After 30 min, samples were subjected to flow cytometry using a FACSCanto II (BD Bioscience) to assess PI fluorescence intensity. Analysis and quantification of the sub-G 0 /G 1 population was completed using FlowJo Software (TreeStar, Ashland, OR, USA).…”

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confidence: 99%

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MLN4924 induces Noxa upregulation in acute myelogenous leukemia and synergizes with Bcl-2 inhibitors

et al. 2015

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MLN4924 (pevonedistat), an inhibitor of the Nedd8 activating enzyme (NAE), has exhibited promising clinical activity in acute myelogenous leukemia (AML). Here we demonstrate that MLN4924 induces apoptosis in AML cell lines and clinical samples via a mechanism distinct from those observed in other malignancies. Inactivation of E3 cullin ring ligases (CRLs) through NAE inhibition causes accumulation of the CRL substrate c-Myc, which transactivates the PMAIP1 gene encoding Noxa, leading to increased Noxa protein, Bax and Bak activation, and subsequent apoptotic changes. Importantly, c-Myc knockdown diminishes Noxa induction; and Noxa siRNA diminishes MLN4924-induced killing. Because Noxa also neutralizes Mcl-1, an anti-apoptotic Bcl-2 paralog often upregulated in resistant AML, further experiments have examined the effect of combining MLN4924 with BH3 mimetics that target other anti-apoptotic proteins. In combination with ABT-199 or ABT-263 (navitoclax), MLN4924 exerts a synergistic cytotoxic effect. Collectively, these results provide new insight into MLN4924-induced engagement of the apoptotic machinery that could help guide further exploration of MLN4924 for AML.

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“…Significance was ascertained using the unpaired one-way ANOVA test (*p < 0.05, *p < 0.01, and ***p < 0.001) (n = 3). During early apoptosis, the integrity of the cell membrane is lost and phosphatidylserine (PS) is exposed for Annexin V binding (21). A significant number of SKOV3 cells were stained positive for Annexin V, when examined under immunofluorescence microscope, suggesting that the cell membrane integrity was no longer intact as Annexin V labeled with FITC was able to bind to PS, which is usually present on the intracellular leaflet of the healthy cells.…”

Section: Discussionmentioning

confidence: 99%

Human c1q induces apoptosis in an ovarian cancer cell line via tumor necrosis factor pathway

Kaur

Sultan

Murugaiah

et al. 2017

Molecular Immunology

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Phosphatidylserine exposure during apoptosis reflects bidirectional trafficking between plasma membrane and cytoplasm

Cited by 173 publications

References 42 publications

Autophagic vesicles on mature human reticulocytes explain phosphatidylserine-positive red cells in sickle cell disease

Autophagic vesicles on mature human reticulocytes explain phosphatidylserine-positive red cells in sickle cell disease

MLN4924 induces Noxa upregulation in acute myelogenous leukemia and synergizes with Bcl-2 inhibitors

Human c1q induces apoptosis in an ovarian cancer cell line via tumor necrosis factor pathway

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