Vps52p, Vps53p, and Vps54p Form a Novel Multisubunit Complex Required for Protein Sorting at the Yeast Late Golgi

Conibear, Elizabeth; Stevens, Tom H.

doi:10.1091/mbc.11.1.305

Cited by 266 publications

(355 citation statements)

References 82 publications

(121 reference statements)

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“…Cells lacking these proteins display high levels of CPY secretion and defects in the stability and distribution of several late Golgi proteins, including the Vps10p CPY receptor. Vps52p, Vps53p and Vps54p are thought to be required for correct retrograde sorting from the PVC back to the late Golgi compartment (Conibear and Stevens, 2000).…”

Section: Some Deletants Display Cpy Secretion But No P2 Cpy Accumulationmentioning

confidence: 99%

“…It is not yet entirely clear whether this pathway originates from early or late endosomes (Galan et al, 2001;Lewis et al, 2000;Panek et al, 2000;Wiederkehr et al, 2000). The distribution of Tlg2p has been reported to overlap with those of TGN and endosomal markers (Abeliovich et al, 1998;Conibear and Stevens, 2000;Holthuis et al, 1998;Panek et al, 2000;Séron et al, 1998).…”

Section: Some Deletants Display Cpy Secretion But No P2 Cpy Accumulationmentioning

confidence: 99%

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Mutants defective in secretory/vacuolar pathways in the EUROFAN collection of yeast disruptants

Avaro

Belgareh‐Touzé

Sibella-Argüelles

et al. 2002

Yeast

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We have screened the EUROFAN (European Functional Analysis Network) deletion strain collection for yeast mutants defective in secretory/vacuolar pathways and/or associated biochemical modifications. We used systematic Western immunoblotting to analyse the electrophoretic pattern of several markers of the secretory/vacuolar pathways, the soluble a-factor, the periplasmic glycoprotein invertase, the plasma membrane GPIanchored protein Gas1p, and two vacuolar proteins, the soluble carboxypeptidase Y and the membrane-bound alkaline phosphatase, which are targeted to the vacuole by different pathways. We also used colony immunoblotting to monitor the secretion of carboxypeptidase Y into the medium, to identify disruptants impaired in vacuolar targeting. We identified 25 mutants among the 631 deletion strains. Nine of these mutants were disrupted in genes identified in recent years on the basis of their involvement in trafficking (VPS53, VAC7, VAM6, APM3, SYS1), or glycosylation (ALG12, ALG9, OST4, ROT2). Three of these genes were identified on the basis of trafficking defects by ourselves and others within the EUROFAN project (TLG2, RCY1, MON2). The deletion of ERV29, which encodes a COPII vesicle protein, impaired carboxypeptidase Y trafficking from the endoplasmic reticulum to the Golgi apparatus. We also identified eight unknown ORFs, the deletion of which reduced Golgi glycosylation or impaired the Golgi to vacuole trafficking of carboxypeptidase Y. YJR044c, which we identified as a new VPS gene, encodes a protein with numerous homologues of unknown function in sequence databases.

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Section: Some Deletants Display Cpy Secretion But No P2 Cpy Accumulationmentioning

confidence: 99%

Section: Some Deletants Display Cpy Secretion But No P2 Cpy Accumulationmentioning

confidence: 99%

Mutants defective in secretory/vacuolar pathways in the EUROFAN collection of yeast disruptants

Avaro

Belgareh‐Touzé

Sibella-Argüelles

et al. 2002

Yeast

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“…The exocyst (sec6/8 complex), composed of eight proteins, is thought to help recruit Golgiderived vesicles to the plasma membrane at the final step of the secretory pathway (Hsu et al, 1996;TerBush et al, 1996;Kee et al, 1997). The multisubunit TRAPP I and Vps52/ 53/54 complexes are believed to serve analogous functions during ER-to-Golgi and endosome-to-Golgi trafficking, respectively (Conibear and Stevens, 2000;Sacher et al, 2001). The eight-component mammalian conserved oligomeric Golgi (COG) complex and the homologous Sec34/35 complex in yeast have been proposed to assist in Golgi vesicle targeting VanRheenen et al, 1998;Walter et al, 1998;VanRheenen et al, 1999;Sacher et al, 2001;Whyte and Munro, 2001;Ungar et al, 2002).…”

Section: Introductionmentioning

confidence: 99%

TheDrosophila Cog5Homologue Is Required for Cytokinesis, Cell Elongation, and Assembly of Specialized Golgi Architecture during Spermatogenesis

Farkas

Giansanti

Gatti

et al. 2003

MBoC

108

149

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The multisubunit conserved oligomeric Golgi (COG) complex has been shown previously to be involved in Golgi function in yeast and mammalian tissue culture cells. Despite this broad conservation, several subunits, including Cog5, were not essential for growth and showed only mild effects on secretion when mutated in yeast, raising questions about what functions these COG complex subunits play in the life of the cell. Here, we show that function of the gene four way stop (fws), which encodes the Drosophila Cog5 homologue, is necessary for dramatic changes in cellular and subcellular morphology during spermatogenesis. Loss-of-function mutations in fws caused failure of cleavage furrow ingression in dividing spermatocytes and failure of cell elongation in differentiating spermatids and disrupted the formation and/or stability of the Golgibased spermatid acroblast. Consistent with the lack of a growth defect in yeast lacking Cog5, animals lacking fws function were viable, although males were sterile. Fws protein localized to Golgi structures throughout spermatogenesis. We propose that Fws may directly or indirectly facilitate efficient vesicle traffic through the Golgi to support rapid and extensive increases in cell surface area during spermatocyte cytokinesis and polarized elongation of differentiating spermatids. Our study suggests that Drosophila spermatogenesis can be an effective sensitized genetic system to uncover in vivo functions for proteins involved in Golgi architecture and/or vesicle transport.

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“…In yeast, Vps53 is a subunit of the Golgi-associated retrograde protein complex, which is involved in retrograde transport from the early and late endosome to the late Golgi. 26 Human Vps53 or HCCS1 was shown to have analogous characteristics to the yeast homologue and co-localized with mannose-6-phosphate receptor, 27 which is the primary receptor for the lysosomal aspartyl protease cathepsin D. 28 Based on these observations, one may conceive that overexpressed HCCS1 induces the efflux of cathepsin D by executing an abnormal transport function in the endosomal/lysosomal system. However, the mechanism by which overexpressed HCCS1 induces the elevation of intracellular calcium is not yet clear.…”

Section: Discussionmentioning

confidence: 99%

HCCS1 overexpression induces apoptosis via cathepsin D and intracellular calcium, and HCCS1 disruption in mice causes placental abnormality

Gan

Zhao

et al. 2008

Cell Death Differ

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Hepatocellular carcinoma suppressor 1 (HCCS1) was discovered as a novel tumor suppressor gene. We recently observed that adenovirus-mediated gene transfer of HCCS1 leads to cytotoxicity to human hepatocarcinoma cells. Here, we have demonstrated that adenovirus-mediated overexpression of HCCS1 induces apoptosis in hepatocarcinoma cells and have further characterized the apoptotic cascade. The results showed that lysosomal cathepsin D is released into the cytosol in response to HCCS1 overexpression and consequently triggers Bax insertion into the mitochondrial membrane, which leads to the release of cytochrome c. In addition, HCCS1 overexpression can induce an increase in intracellular free Ca 2 þ concentration, which also results in cytochrome c release. The released cytochrome c activates downstream caspases, leading to the occurrence of the late stages of apoptosis. Moreover, we demonstrated that the disruption of HCCS1 in mice leads to embryonic lethality, accompanied by abnormal labyrinth architecture resulting from the excessive proliferation of trophoblast cells in the placenta. These results suggest that HCCS1 plays a role in apoptosis regulation and development.

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Vps52p, Vps53p, and Vps54p Form a Novel Multisubunit Complex Required for Protein Sorting at the Yeast Late Golgi

Cited by 266 publications

References 82 publications

Mutants defective in secretory/vacuolar pathways in the EUROFAN collection of yeast disruptants

Mutants defective in secretory/vacuolar pathways in the EUROFAN collection of yeast disruptants

TheDrosophila Cog5Homologue Is Required for Cytokinesis, Cell Elongation, and Assembly of Specialized Golgi Architecture during Spermatogenesis

HCCS1 overexpression induces apoptosis via cathepsin D and intracellular calcium, and HCCS1 disruption in mice causes placental abnormality

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