Crystal structures of saposins A and C

Ahn, Victoria E.; Leyko, Paul; Alattia, Jean‐René; Chen, Lu; Privé, Gilbert G.

doi:10.1110/ps.062256606

Cited by 88 publications

(122 citation statements)

References 48 publications

(78 reference statements)

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“…Saposins A, C, and D have high homology to each other, with pairwise sequence identities ranging from 34% to 39%. Saposin B is more distantly related, with sequence identities of 22%, 15%, and 21% with saposins A, C, and D, respectively (35). The more important difference is in the lipid activation mechanism.…”

Section: Saposin B Most Efficiently Enhances Cd1d Lipid Presentation mentioning

confidence: 99%

“…The affinity of saposin B for lipid bilayers is low at both neutral and acidic pH, consistent with its function as an extractor/solubilizer that has only transient interactions with the membrane. Furthermore, low pH affects the structure of saposin B differently from the way it affects saposin A or C (35). Saposins A and C, as well as most other saposin-like proteins, have a compact, monomeric fold that buries a small hydrophobic core, whereas saposin B, like GM2 activator protein, has a major conformational variant that forms a homodimer that has a large hydrophobic cavity (26).…”

Section: Saposin B Most Efficiently Enhances Cd1d Lipid Presentation mentioning

confidence: 99%

“…Saposins A and C, as well as most other saposin-like proteins, have a compact, monomeric fold that buries a small hydrophobic core, whereas saposin B, like GM2 activator protein, has a major conformational variant that forms a homodimer that has a large hydrophobic cavity (26). For saposins A and C, low pH and the presence of detergent is required for dimer formation, whereas saposin B is dimeric at both neutral and low pH and in the presence or absence of detergent (35). These data again support the argument that the two categories of saposins interact differently with lipids in a manner relevant to the superior capacity of saposin B to facilitate lipid binding to CD1d.…”

Section: Saposin B Most Efficiently Enhances Cd1d Lipid Presentation mentioning

confidence: 99%

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Saposin B is the dominant saposin that facilitates lipid binding to human CD1d molecules

Yuan

Tsang

et al. 2007

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

102

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CD1d molecules bind lipid antigens in the endocytic pathway, and access to the pathway is important for the development of CD1d-restricted natural killer T (NKT) cells. Saposins, derived from a common precursor, prosaposin, are small, heat-stable lysosomal glycoproteins required for lysosomal degradation of sphingolipids. Expression of prosaposin is required for efficient lipid binding and recognition of human CD1d molecules by NKT cells. Despite high sequence homology among the four saposins, they have different specificities for lipid substrates and different mechanisms of action. To determine the saposins involved in promoting lipid binding to CD1d, we expressed prosaposin deletion mutants lacking individual saposins in prosaposin-negative, CD1d-positive cells. No individual saposin proved to be absolutely essential, but the absence of saposin B resulted in the lowest recognition of α-galactosylceramide by NKT cells. When recombinant exogenous saposins were added to the prosaposin-negative cells, saposin B was the most efficient in restoring CD1d recognition. Saposin B was also the most efficient in mediating α-galactosylceramide binding to recombinant plate-bound CD1d and facilitating NKT cell activation. Saposin B could also mediate lipid binding to soluble CD1d molecules in a T cell-independent assay. The optimal pH for saposin B-mediated lipid binding to CD1d, pH 6, is higher than that of lysosomes, suggesting that saposin B may facilitate lipid binding to CD1d molecules throughout the endocytic pathway.

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Section: Saposin B Most Efficiently Enhances Cd1d Lipid Presentation mentioning

confidence: 99%

Section: Saposin B Most Efficiently Enhances Cd1d Lipid Presentation mentioning

confidence: 99%

Section: Saposin B Most Efficiently Enhances Cd1d Lipid Presentation mentioning

confidence: 99%

See 1 more Smart Citation

Saposin B is the dominant saposin that facilitates lipid binding to human CD1d molecules

Yuan

Tsang

et al. 2007

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

102

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“…sapC was labeled with the Alexa Fluor 546 (A546) fluorophore at residue 22. This position is in a short loop between helices ␣1 and ␣2 of the protein and is the site normally glycosylated in the natural protein (24). GCase was chemically labeled using an amine-reactive Alexa Fluor 488 (A488) succinimidyl conjugate.…”

mentioning

confidence: 99%

Molecular imaging of membrane interfaces reveals mode of β-glucosidase activation by saposin C

Alattia

Shaw²,

Yip³

et al. 2007

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

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Acid ␤-glucosidase (GCase) is a soluble lysosomal enzyme responsible for the hydrolysis of glucose from glucosylceramide and requires activation by the small nonenzymatic protein saposin C (sapC) to gain access to the membrane-embedded glycosphingolipid substrate. We have used in situ atomic force microscopy (AFM) with simultaneous confocal and epifluorescence microscopies to investigate the interactions of GCase and sapC with lipid bilayers. GCase binds to sites on membranes transformed by sapC, and enzyme activity occurs at loci containing both GCase and sapC. Using FRET, we establish the presence of GCase/sapC and GCase/ product contacts in the bilayer. These data support a mechanism in which sapC locally alters regions of bilayer for subsequent attack by the enzyme in stably bound protein complexes.atomic force microscopy ͉ confocal microscopy ͉ FRET ͉ interfacial catalysis ͉ lipid storage disease

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“…Interestingly, the saposin-like domain of CDNF crystallized as a dimer at pH 4.6, whereas the full-length, mature MANF crystallized as a monomer at neutral pH (Parkash et al, 2009). Saposin C and Saposin A form oligomers in the presence of a detergent at low pH 4.8 (Ahn et al, 2006). Acidic pH also increases the ability of Saposin C and Saposin D to bind lipid vesicles and destabilize phospholipid-containing membranes (Vaccaro et al, 1995).…”

Section: Two Domains-two Activities?mentioning

confidence: 99%

Novel CDNF/MANF family of neurotrophic factors

Lindholm

Saarma

2010

Developmental Neurobiology

174

136

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Current therapeutic interventions for neurodegenerative diseases alleviate only disease symptoms, while treatments that could stop or reverse actual degenerative processes are not available. Parkinson's disease (PD) is a movement disorder with characteristic degeneration of dopaminergic neurons in the midbrain. Few neurotrophic factors (NTFs) that promote survival, maintenance, and differentiation of affected brain neurons are considered as potential therapeutic agents for the treatment of neurodegenerative diseases. Thus, it is important to search and study new NTFs that could also be used in therapy. In this review, we discuss novel evolutionary conserved family of NTFs consisting of two members in the vertebrates, cerebral dopamine neurotrophic factor (CDNF) and mesencephalic astrocyte-derived neurotrophic factor (MANF). Invertebrates, including Drosophila and Caenorhabditis have a single protein homologous to vertebrate CDNF/ MANF. Characteristic feature of these proteins is eight structurally conserved cysteine residues, which determine the protein fold. The crystal structure analysis revealed that CDNF and MANF consist of two domains; an amino-terminal saposin-like domain that may interact with lipids or membranes, and a presumably unfolded carboxy-terminal domain that may protect cells against endoplasmic reticulum stress. CDNF and MANF protect midbrain dopaminergic neurons and restore motor function in 6-hydroxydopamine rat model of PD in vivo. In line, Drosophila MANF is needed for the maintenance of dopaminergic neurites and dopamine levels in the fly, suggesting that the function of CDNF/MANF proteins is evolutionary conserved. Future studies will reveal the receptors and mode of action of these novel factors, which are potential therapeutic proteins for the treatment of PD. ' 2010 Wiley Periodicals, Inc. Develop Neurobiol 70: 360-371, 2010

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Crystal structures of saposins A and C

Cited by 88 publications

References 48 publications

Saposin B is the dominant saposin that facilitates lipid binding to human CD1d molecules

Saposin B is the dominant saposin that facilitates lipid binding to human CD1d molecules

Molecular imaging of membrane interfaces reveals mode of β-glucosidase activation by saposin C

Novel CDNF/MANF family of neurotrophic factors

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