Integral and Associated Lysosomal Membrane Proteins

Schröder, Bernd; Wrocklage, Christian; Pan, Cuiping; Jäger, Ralf; Kösters, Bernd; Schäfer, Helmut; Elsässer, Hans–Peter; Mann, Matthias; Hasilík, Andrej

doi:10.1111/j.1600-0854.2007.00643.x

Cited by 181 publications

(162 citation statements)

References 48 publications

(59 reference statements)

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“…However, DPP4, CD9, and EPCAM have each been identified in exosomes from a variety of cell types (17-19) (Vesiclepedia database), likely reflecting ambiguity in their membrane associations. Indeed, despite its use as a marker of apical membrane polarity, DPP4 is a well-established lysosomal membrane component (20).…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Protein composition of the hepatitis A virus quasi-envelope

McKnight

Xie

González‐López

et al. 2017

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

123

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The Picornaviridae are a diverse family of RNA viruses including many pathogens of medical and veterinary importance. Classically considered "nonenveloped," recent studies show that some picornaviruses, notably hepatitis A virus (HAV; genus Hepatovirus) and some members of the Enterovirus genus, are released from cells nonlytically in membranous vesicles. To better understand the biogenesis of quasienveloped HAV (eHAV) virions, we conducted a quantitative proteomics analysis of eHAV purified from cell-culture supernatant fluids by isopycnic ultracentrifugation. Amino acid-coded mass tagging (AACT) with stable isotopes followed by tandem mass spectrometry sequencing and AACT quantitation of peptides provided unambiguous identification of proteins associated with eHAV versus unrelated extracellular vesicles with similar buoyant density. Multiple peptides were identified from HAV capsid proteins (53.7% coverage), but none from nonstructural proteins, indicating capsids are packaged as cargo into eHAV vesicles via a highly specific sorting process. Other eHAVassociated proteins (n = 105) were significantly enriched for components of the endolysosomal system (>60%, P < 0.001) and included many common exosome-associated proteins such as the tetraspanin CD9 and dipeptidyl peptidase 4 (DPP4) along with multiple endosomal sorting complex required for transport III (ESCRT-III)-associated proteins. Immunoprecipitation confirmed that DPP4 is displayed on the surface of eHAV produced in cell culture or present in sera from humans with acute hepatitis A. No LC3-related peptides were identified by mass spectrometry. RNAi depletion studies confirmed that ESCRT-III proteins, particularly CHMP2A, function in eHAV biogenesis. In addition to identifying surface markers of eHAV vesicles, the results support an exosome-like mechanism of eHAV egress involving endosomal budding of HAV capsids into multivesicular bodies.exosome | multivesicular body | ESCRT | extracellular vesicle | picornavirus T he Picornaviridae are a large and diverse family of positivestrand RNA viruses that include numerous pathogens (1). Classically considered "nonenveloped," these viruses package their single-stranded genomes within stable icosahedral protein capsids that are released from cells following cell lysis. However, recent work has revealed that several picornaviruses gain egress from cells in a nonlytic fashion within the lumen of extracellular vesicles shed from the cell. Most notably, hepatitis A virus (HAV; genus Hepatovirus), an important cause of enterically transmitted hepatitis in humans, replicates without cytopathic effect and is released from cells as membrane-wrapped, "quasienveloped" (eHAV) virions similar in size and density to exosomes (2). eHAV virions have been identified in sera collected from persons with acute hepatitis A, as well as in supernatant fluids of infected cell cultures. These virions are completely cloaked in host-derived membranes that protect the capsid from neutralizing antibody until the quasi-envelope is degraded wi...

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Section: Resultsmentioning

confidence: 99%

“…3). This includes DPP4, which, although an integral apical transmembrane protein, is also associated with lysosomes (20). No array of proteins has been shown to be completely specific for exosomes versus other types of extracellular vesicles formed by outward budding at the plasma membrane rather than inward budding into MVBs (17).…”

Section: Discussionmentioning

confidence: 99%

Protein composition of the hepatitis A virus quasi-envelope

McKnight

Xie

González‐López

et al. 2017

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

123

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“…Screens employing two distinct custom shRNA libraries were performed to identify genes involved in noncleavable linker maytansine ADC (anti-CD70 Ab-MCC-DM1) catabolite transport from the lysosome to cytoplasm. Library 1 contained genes annotated as membrane proteins, predominantly cell surface proteins, while cancerres.aacrjournals.org Downloaded from library 2 was designed to include genes annotated to have transporter function or lysosomal localization (20)(21)(22), approximately 35 amino acid transporter genes, and genes that regulate lysosomal function consisting of 14 lysosmal ATPase subunits. The shRNA libraries were screened in 786-0 cells using cell survival as a readout (Fig.…”

Section: Shrna Screens Identified Cd70 and Slc46a3 As Critical Mediatmentioning

confidence: 99%

SLC46A3 Is Required to Transport Catabolites of Noncleavable Antibody Maytansine Conjugates from the Lysosome to the Cytoplasm

et al. 2015

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Antibody-drug conjugates (ADC) target cytotoxic drugs to antigen-positive cells for treating cancer. After internalization, ADCs with noncleavable linkers are catabolized to amino acidlinker-warheads within the lysosome, which then enter the cytoplasm by an unknown mechanism. We hypothesized that a lysosomal transporter was responsible for delivering noncleavable ADC catabolites into the cytoplasm. To identify candidate transporters, we performed a phenotypic shRNA screen with an anti-CD70 maytansine-based ADC. This screen revealed the lysosomal membrane protein SLC46A3, the genetic attenuation of which inhibited the potency of multiple noncleavable antibodymaytansine ADCs, including ado-trastuzumab emtansine. In contrast, the potencies of noncleavable ADCs carrying the structurally distinct monomethyl auristatin F were unaffected by SLC46A3 attenuation. Structure-activity experiments suggested that maytansine is a substrate for SLC46A3. Notably, SLC46A3 silencing led to relative increases in catabolite concentrations in the lysosome. Taken together, our results establish SLC46A3 as a direct transporter of maytansine-based catabolites from the lysosome to the cytoplasm, prompting further investigation of SLC46A3 as a predictive response marker in breast cancer specimens. Cancer Res; 75(24); 5329-40. Ó2015 AACR.

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“…These catabolic functions of lysosomes are catalyzed by more than 50 different soluble acid hydrolases and accessory activator proteins (29). The hydrolases are separated from the cytoplasm by a lysosomal membrane composed of about 140 highly glycosylated membrane proteins (2,42,43). In addition, the lipid composition of lysosomal membranes differs from that of plasma membranes or other limiting membranes of subcellular compartments and is characterized by a low cholesterol and an enriched anionic lipid content (44).…”

mentioning

confidence: 99%

Mannose 6 Dephosphorylation of Lysosomal Proteins Mediated by Acid Phosphatases Acp2 and Acp5

Makrypidi

Damme

Müller‐Loennies

et al. 2012

Molecular and Cellular Biology

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Mannose 6-phosphate (Man6P) residues represent a recognition signal required for efficient receptor-dependent transport of soluble lysosomal proteins to lysosomes. Upon arrival, the proteins are rapidly dephosphorylated. We used mice deficient for the lysosomal acid phosphatase Acp2 or Acp5 or lacking both phosphatases (Acp2/Acp5 ؊/؊ ) to examine their role in dephosphorylation of Man6P-containing proteins. Two-dimensional (2D) Man6P immunoblot analyses of tyloxapol-purified lysosomal fractions revealed an important role of Acp5 acting in concert with Acp2 for complete dephosphorylation of lysosomal proteins. The most abundant lysosomal substrates of Acp2 and Acp5 were identified by Man6P affinity chromatography and mass spectrometry. Depending on the presence of Acp2 or Acp5, the isoelectric point of the lysosomal cholesterol-binding protein Npc2 ranged between 7.0 and 5.4 and may thus regulate its interaction with negatively charged lysosomal membranes at acidic pH. Correspondingly, unesterified cholesterol was found to accumulate in lysosomes of cultured hepatocytes of Acp2/Acp5 ؊/؊ mice. The data demonstrate that dephosphorylation of Man6P-containing lysosomal proteins requires the concerted action of Acp2 and Acp5 and is needed for hydrolysis and removal of degradation products.

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Integral and Associated Lysosomal Membrane Proteins

Cited by 181 publications

References 48 publications

Protein composition of the hepatitis A virus quasi-envelope

Protein composition of the hepatitis A virus quasi-envelope

SLC46A3 Is Required to Transport Catabolites of Noncleavable Antibody Maytansine Conjugates from the Lysosome to the Cytoplasm

Mannose 6 Dephosphorylation of Lysosomal Proteins Mediated by Acid Phosphatases Acp2 and Acp5

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