Autoinhibition of the ligand-binding site of GGA1/3 VHS domains by an internal acidic cluster-dileucine motif

Doray, Balraj; Bruns, Kerry A.; Ghosh, Pradipta; Kornfeld, Stuart

doi:10.1073/pnas.082235699

Cited by 79 publications

(116 citation statements)

References 28 publications

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“…In this model, GGA is displaced by AP-1 through a phosphorylation statedependent structural change. Internal ACLL motifs in the hinge region of human GGA1 and GGA3 are thought to mediate this structural change (Doray et al, 2002c). Through the characterization of dGGA and Drosophila AP-1 (dAP-1) in the current study (Fig.…”

Section: Both Dgga and Dap-1 Contribute To Lerp Traffickingmentioning

confidence: 99%

Functional characterization of protein-sorting machineries at the trans-Golgi network in Drosophila melanogaster

Kametaka

Sawada

Bonifacino

et al. 2010

Journal of Cell Science

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SummaryTargeting of proteins to their final destination is a prerequisite for living cells to maintain their homeostasis. Clathrin functions as a coat that forms transport carriers called clathrin-coated vesicles (CCVs) at the plasma membrane and post-Golgi compartments. In this study, we established an experimental system using Schneider S2 cells derived from the fruit fly, Drosophila melanogaster, as a model system to study the physiological roles of clathrin adaptors, and to dissect the processes of CCV formation. We found that a clathrin adaptor Drosophila GGA (dGGA), a homolog of mammalian GGA proteins, localizes to the trans-Golgi network (TGN) and is capable of recruiting clathrin from the cytosol onto TGN membranes. dGGA itself is recruited from the cytosol to the TGN in an ARF1 small GTPase (dARF79F)-dependent manner. dGGA recognizes the cytoplasmic acidic-cluster-dileucine (ACLL) sorting signal of Lerp (lysosomal enzyme receptor protein), a homolog of mammalian mannose 6-phosphate receptors. Moreover, both dGGA and another type of TGN-localized clathrin adaptor, AP-1 (adaptor protein-1 complex), are shown to be involved in the trafficking of Lerp from the TGN to endosomes and/or lysosomes. Taken together, our findings indicate that the protein-sorting machinery in fly cells is well conserved relative to that in mammals, enabling the use of fly cells to dissect CCV biogenesis and clathrin-dependent protein trafficking at the TGN of higher eukaryotes.

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Section: Both Dgga and Dap-1 Contribute To Lerp Traffickingmentioning

confidence: 99%

Functional characterization of protein-sorting machineries at the trans-Golgi network in Drosophila melanogaster

Kametaka

Sawada

Bonifacino

et al. 2010

Journal of Cell Science

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“…Later, the GGA-VHS domains were shown to be able to interact with the ACLL sequence in b-secretase (BACE), which is responsible for the b-site cleavage of the amyloid precursor protein to yield the Ab peptide, and that in sorLA, which is homologous to sortilin (He et al, 2002;Jacobsen et al, 2002). Furthermore, it is also noteworthy that the VHS domains are able to interact with potential ACLL sequences that are found in the hinge regions of GGA1 and GGA3 but not in GGA2 (Doray et al, 2002a) (see below). Despite its binding to cargo proteins found in the TGN, the VHS domain appears not to be the major determinant of TGN association of GGAs, because the domain alone expressed in cells is predominantly cytosolic and because GGA3S, which is defective in ACLL binding, shows TGN localization.…”

Section: (I) Vhs Domainmentioning

confidence: 93%

“…2). Phosphorylation of a serine residue at position -3 results in autoinhibition of the VHS domain from interacting with the ACLL sequences of cargo proteins (Doray et al, 2002a). Based on the VHSpeptide complex structures, however, the serine residue is predicted to be placed out of the conventional ACLL binding site, suggesting that the phosphorylated serine is recognized by another part of the VHS domain.…”

Section: (I) Vhs Domainmentioning

confidence: 99%

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The Structure and Function of GGAs, the Traffic Controllers at the TGN Sorting Crossroads

Nakayama

Wakatsuki

2003

Cell Struct. Funct.

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ABSTRACT. GGAs (Golgi-localizing, g-adaptin ear homology domain, ARF-binding proteins) are a family of monomeric clathrin adaptor proteins that are conserved from yeasts to humans. Data published during the past four years have provided detailed pictures of the localization, domain organization and structure-function relationships of GGAs. GGAs possess four conserved functional domains, each of which interacts with cargo proteins including mannose 6-phosphate receptors, the small GTPase ARF, clathrin, or accessory proteins including Rabaptin-5 and g-synergin. Together with or independent of the adaptor protein complex AP-1, GGAs regulate selective transport of cargo proteins, such as mannose 6-phosphate receptors, from the trans-Golgi network to endosomes mediated by clathrin-coated vesicles.

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“…The hinge region contains a clathrin-binding sequence and is responsible for clathrin association (8,11,13,14). The hinge region of GGA1 and GGA3 also contains an autoinhibitory sequence that, when phosphorylated by casein kinase II, blocks receptor binding to the VHS domain (15). The GAE domain is responsible for binding accessory proteins, including Rabaptin-5 and ␥-synergin (2,5,8,16).…”

mentioning

confidence: 99%

Structure of the GAT domain of human GGA1: A syntaxin amino-terminal domain fold in an endosomal trafficking adaptor

Suer

Misra

Saidi

et al. 2003

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

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The Golgi-associated, ␥-adaptin homologous, ADP-ribosylation factor (ARF)-interacting proteins (GGAs) are adaptors that sort receptors from the trans-Golgi network into the endosomal͞lyso-somal pathway. The GGAs and TOM1 (GAT) domains of the GGAs are responsible for their ARF-dependent localization. The 2.4-Å crystal structure of the GAT domain of human GGA1 reveals a three-helix bundle, with a long N-terminal helical extension that is not conserved in GAT domains that do not bind ARF. The ARF binding site is located in the N-terminal extension and is separate from the core three-helix bundle. An unanticipated structural similarity to the N-terminal domain of syntaxin 1a was discovered, comprising the entire three-helix bundle. A conserved binding site on helices 2 and 3 of the GAT domain three-helix bundle is predicted to interact with coiled-coil-containing proteins. We propose that the GAT domain is descended from the same ancestor as the syntaxin 1a N-terminal domain, and that both protein families share a common function in binding coiled-coil domain proteins.

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Autoinhibition of the ligand-binding site of GGA1/3 VHS domains by an internal acidic cluster-dileucine motif

Cited by 79 publications

References 28 publications

Functional characterization of protein-sorting machineries at the trans-Golgi network in Drosophila melanogaster

Functional characterization of protein-sorting machineries at the trans-Golgi network in Drosophila melanogaster

The Structure and Function of GGAs, the Traffic Controllers at the TGN Sorting Crossroads

Structure of the GAT domain of human GGA1: A syntaxin amino-terminal domain fold in an endosomal trafficking adaptor

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