Thermal Stabilities of Brain Spectrin and the Constituent Repeats of Subunits

An, Xiuli; Zhang, Xihui; Salomao, Marcela A.; Guo, Xinhua; Yang, Yang; Wu, Yu; Gratzer, Walter; Baines, Anthony J.; Mohandas, Narla

doi:10.1021/bi061368x

Cited by 30 publications

(39 citation statements)

References 38 publications

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“…27 Thus, the helix C, linker, and interhelix loops (particularly the B-C loop), are sites that readily accommodate modification without disruption of the structural repeat. Although the linker provides a crucial bridge coupling the folding and unfolding of paired repeats to each other, 42 we propose that the linker has additional roles. Specifically, we propose that the spectrin di-repeat unit represents a novel and here-to-fore unappreciated general protein-protein interaction motif.…”

Section: Discussionmentioning

confidence: 90%

“…Previously determined spectrin di-repeat structures 36,38 indicate that the side-chains of these 3 residues form a tightly packed hydrophobic core that has been proposed to contribute to peptide folding and stability and possibly to its physiologic role. 23,26,41,42 However, we find that the absence of Trp and the Trp-His couple in ␤I-15 is not critical for stability of this di-repeat, nor does it modify ankyrin recognition (Figure 1). Furthermore, we find in our structure that the hydrophobic core of ␤I-15 is tightly packed, similar to that of other spectrin repeats, regardless of its lack of the invariant Trp residue in helix A.…”

Section: Org Frommentioning

confidence: 80%

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The structure of the ankyrin-binding site of β-spectrin reveals how tandem spectrin-repeats generate unique ligand-binding properties

Stabach¹,

Simonović²,

Ranieri

et al. 2009

Blood

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Spectrin and ankyrin participate in membrane organization, stability, signal transduction, and protein targeting; their interaction is critical for erythrocyte stability. Repeats 14 and 15 of ␤I-spectrin are crucial for ankyrin recognition, yet the way spectrin binds ankyrin while preserving its repeat structure is unknown. We have solved the crystal structure of the ␤I-spectrin 14,15 di-repeat unit to 2.1 Å resolution and found 14 residues critical for ankyrin binding that map to the end of the helix C of repeat 14, the linker region, and the B-C loop of repeat 15. The tilt (64°) across the 14,15 linker is greater than in any published di-repeat structure, suggesting that the relative positioning of the two repeats is important for ankyrin binding. We propose that a lack of structural constraints on linker and inter-helix loops allows proteins containing spectrin-like di-repeats to evolve diverse but specific ligand-recognition sites without compromising the structure of the repeat unit. The linker regions between repeats are thus critical determinants of both spectrin's flexibility and polyfunctionality. The putative coupling of flexibility and ligand binding suggests a mechanism by which spectrin might participate in mechanosensory regulation. (Blood. 2009;113:5377-5384) IntroductionFirst discovered in the human erythrocyte and closely associated with a variety of familial hemolytic anemias, the spectrin-ankyrin cytoskeleton has emerged as the classical paradigm of a polyfunctional organizing membrane scaffold. Ubiquitous in higher eukaryotes, the spectrin-ankyrin skeleton contributes to membrane stability, the organization of membrane proteins and lipids, the recruitment to membranes of cytosolic proteins and signaling complexes, the tethering of organized protein mosaics to filamentous actin or to the motors effecting microtubule-directed transport, and the facilitated transport of membrane proteins through the secretory and endocytic pathways. 1 Reflecting these diverse but fundamental roles, hereditary or experimental disruption of spectrin or ankyrin leads to many pathologies, including hemolytic disease, 2 embryonic lethality, cancer and developmental defects, 3 pump and channel failures and endoplasmic reticulum (ER) retention disorders, 4 neuromuscular syndromes and sudden cardiac death. 5,6 The participation of spectrin and ankyrin in so many cellular processes reflects their ability to organize multiple membrane and cytosolic proteins and lipids into membrane microdomains, linking them to the filamentous skeleton. Polyfunctionality is a critical attribute of both proteins. Ankyrins derive this capacity largely by the juxtaposition of multiple 33-residue repeat units, each composed of 2 helices linked by a ␤-turn. 7 Selectivity is achieved by minor sequence variation within the ␤-turn of each ankyrin-repeat and by the juxtaposition of repeats with differing sequence. Less is known about how spectrin binds its ligands with high affinity and specificity. In humans, there are 7 spectrin genes encoding 5...

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Section: Discussionmentioning

confidence: 90%

Section: Org Frommentioning

confidence: 80%

The structure of the ankyrin-binding site of β-spectrin reveals how tandem spectrin-repeats generate unique ligand-binding properties

Stabach¹,

Simonović²,

Ranieri

et al. 2009

Blood

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“…D-DЈ, ␣wt, weeP␣/TM6; ␣1cx, is weeP␣/P{␣-spec R22S } ␣-spec rg41 . E, overexpression of wild-type ␣-spectrin (MTDGal4ϾUAS-␣-spectrin 37 ). F-FЉ, egg chambers from ␣-spectrin R22S rescued flies expressing 2 or 3 copies of the ␣-spec R22S transgene stained with 1B1 that exhibit gaps in the normally continuous follicle cell monolayer (arrows, other labels as in B).…”

Section: Discussionmentioning

confidence: 99%

“…We therefore overexpressed wild-type ␣-spectrin in the germline in a wild-type ␣-spectrin background using the Gal4/UAS system (42) with the MTD-Gal4 driver. Staining MTD-Gal4ϾUAS-␣-spectrin 37 ovarioles for 1B1 reveals fusomes of normal complexity (Fig. 6E).…”

Section: Characterizing the Fly Spectrin Head-to-head Interactions-mentioning

confidence: 97%

Spectrin Tetramer Formation Is Not Required for Viable Development in Drosophila

Khanna

Mattie

Browder

et al. 2015

Journal of Biological Chemistry

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Background: Underneath the membrane of most animal cells is a network (membrane skeleton) assembled using tetramers of the protein spectrin. Results: Although spectrins are essential proteins, tetramer formation is surprisingly unimportant for Drosophila development. Conclusion:The major roles of the membrane skeleton do not require a conventional network. Significance: The ubiquitous model of the spectrin-based membrane skeleton has limited applicability.

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“…33,34,40,41 In addition to their principal role as an elastic module, there is increasing evidence that spectrin repeats may also serve as docking sites for cytoskeletal and signal transduction proteins. For example, the repeats of ␣-actinin (a member of spectrin family) have been shown to interact with cytoplasmic domains of integrins 42 and intercellular adhesion molecules.…”

Section: Discussionmentioning

confidence: 99%

Adhesive activity of Lu glycoproteins is regulated by interaction with spectrin

Gauthier

Zhang

et al. 2008

Blood

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The Lutheran (Lu) and Lu(v13) blood group glycoproteins function as receptors for extracellular matrix laminins. Lu and Lu(v13) are linked to the erythrocyte cytoskeleton through a direct interaction with spectrin. However, neither the molecular basis of the interaction nor its functional consequences have previously been delineated. In the present study, we defined the binding motifs of Lu and Lu(v13) on spectrin and identified a functional role for this interaction. We found that the cytoplasmic domains of both Lu and Lu(v13) bound to repeat 4 of the ␣ spectrin chain. The interaction of fulllength spectrin dimer to Lu and Lu(v13) was inhibited by repeat 4 of ␣-spectrin. IntroductionThere is mounting interest in the 2 Lutheran (Lu) red cell transmembrane glycoprotein isoforms that serve as receptors for extracellular matrix laminins. Current evidence indicates that Lu-laminin binding contributes to sickle cell vaso-occlusion. [1][2][3][4][5] Lu-dependent sickle red blood cell adhesion appears to involve epinephrine and cyclic adenosine monophosphate activation, supporting the novel concept that inside-out signaling mechanisms may activate red cell adhesion molecules. 6 Moreover, polycythemia vera red blood cells (RBCs) demonstrate increased adherence to vascular endothelium also mediated by Lu-laminin binding, suggesting that this interaction may contribute to the increased thrombosis observed in this myeloproliferative disorder. 7 Lu first appears on the erythroblast surface late in differentiation, 8 and circulating erythrocytes express 1500 to 4000 copies per cell. 9,10 However, Lu expression is not limited to red cells; the isoforms are also present on vascular endothelial cells and epithelial cells in multiple tissues. 11 Intriguing recent data show that Lu expression is enhanced in various carcinomas and during malignant transformation of epithelial cells, pointing to a possible role in cancer biology. [12][13][14][15] To better understand Lu receptor function(s) in both normal and pathologic states, we are investigating the structural interactions of these transmembrane proteins.The 2 Lu isoforms (85 and 78 kDa) 16 are members of the immunoglobulin superfamily (IgSF). 11 The 85-kDa Lu glycoprotein contains 5 disulfide-bonded extracellular IgSF domains, a single hydrophobic membrane span, and a cytoplasmic domain of 59 residues. 11 Its cytoplasmic tail may function in intracellular signaling and polarization to plasma membrane, as suggested by the presence of the consensus motif for binding of Src homology 3 (SH3) domains, 5 potential phosphorylation sites, 11 and a dileucine motif responsible for regulating basolateral localization of Lu in polarized epithelial cells. 17 The 78-kDa isoform (termed Lu(v13) 18 or B-CAM 13 ), generated by alternative splicing of intron 13, differs from the larger form by having a truncated cytoplasmic tail lacking the proline-rich SH3-binding domain, the dileucine motif, and the 5 phosphorylation sites. 18 Erythrocyte membranes contain 5-to 10-fold more Lu than Lu(v13). 17...

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Thermal Stabilities of Brain Spectrin and the Constituent Repeats of Subunits

Cited by 30 publications

References 38 publications

The structure of the ankyrin-binding site of β-spectrin reveals how tandem spectrin-repeats generate unique ligand-binding properties

The structure of the ankyrin-binding site of β-spectrin reveals how tandem spectrin-repeats generate unique ligand-binding properties

Spectrin Tetramer Formation Is Not Required for Viable Development in Drosophila

Adhesive activity of Lu glycoproteins is regulated by interaction with spectrin

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