Structure of the human lipid exporter ABCB4 in a lipid environment

Olsen, Jeppe; Alam, Amer; Kowal, Julia; Stieger, Bruno; Locher, Kaspar P.

doi:10.1038/s41594-019-0354-3

Cited by 76 publications

(110 citation statements)

References 92 publications

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“…The directions of substrate transport are indicated by solid and dashed red arrows. The structures have the following Protein Data Bank (PDB) accession codes: MalFGK 2 ‐MalE: 2R6G [12]; BtuC 2 D 2 ‐BtuF: 4FI3 [50]; EcfTAA’‐FolT: 4HUQ [14]; Sav1866: 2HYD [15]; TmrAB: 5MKK [51]; TM287/288: 4Q4H [52]; McjD: 4PL0 [53]; PCAT1: 6V9Z [54]; Atm1: 4MYH [55]; MRP1: 5UJA [56]; PrtD: 5L22 [57]; P‐gp: 4M1M [58]; TAP1/2: 5U1D [59]; ABCB4: 6S7P [60]; ABCB8: 5OCH; ABCB10: 3ZDQ [61]; ABCB11: 6LR0 [62]; MsbA: 5TV4 [63]; PglK: 6HRC [64]; YbtPQ: 6P6J [31]; IrtAB: 6TEJ [32]; Rv1819c: 6TQF [33]; ABCD4: 6JBJ [30]; CFTR: 5UAK [65]; SUR1: 6BAA [66]; Wzm‐WztN: 6OIH [25]; TarGH: 6JBH [26]; ABCG5/8: 5DO7 [16]; ABCG2: 6HCO [67]; ABCA1: 5XJY [23]; LptB 2 FG: 5X5Y [17]; MacB: 5LJ7 [21]. ABC, ATP‐binding cassette; β‐jr, β‐jellyroll‐like domain; C, C terminus; CH, coupling helix; CoH, connecting helix; EH, elbow helix; N, N terminus; NBD, nucleotide‐binding domain; P2, extracytoplasmic loop; PG, periplasmic gate helix; PLD, periplasmic domain; TMD, transmembrane domain.…”

Section: Figmentioning

confidence: 99%

Structural and functional diversity calls for a new classification of ABC transporters

et al. 2020

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Members of the ATP‐binding cassette (ABC) transporter superfamily translocate a broad spectrum of chemically diverse substrates. While their eponymous ATP‐binding cassette in the nucleotide‐binding domains (NBDs) is highly conserved, their transmembrane domains (TMDs) forming the translocation pathway exhibit distinct folds and topologies, suggesting that during evolution the ancient motor domains were combined with different transmembrane mechanical systems to orchestrate a variety of cellular processes. In recent years, it has become increasingly evident that the distinct TMD folds are best suited to categorize the multitude of ABC transporters. We therefore propose a new ABC transporter classification that is based on structural homology in the TMDs.

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Section: Figmentioning

confidence: 99%

Structural and functional diversity calls for a new classification of ABC transporters

et al. 2020

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“…Therefore, the ability to image membrane proteins, embedded in lipid nanodisks [98], seems to be very appealing. This system provides a lipid environment, which is considered to be close to native, while still allowing for high-resolution structure determination, as demonstrated by several examples in the ABC-transporter field [7,8,25,56] (Fig. 2).…”

Section: Environment-dependent Biasmentioning

confidence: 99%

“…A range for ABC transporters are now becoming common even without such fiducials [19,22,23,26,42,[44][45][46][47]49,51,56,91,92]. Therefore, it is preferable to avoid antibodies whenever possible to minimize the risk of locking the transporter in a nonphysiological conformation.…”

Section: High Resolution Of Small Particlesmentioning

confidence: 99%

“…Such technology has been shown to enable high‐resolution characterization of as small membrane proteins as, for example, 50‐kDa malaria parasite transporter [18] and has also been successfully applied to several ABC transporters [8,24,54]. On the other hand, resolutions in the 3.1–3.5 Å range for ABC transporters are now becoming common even without such fiducials [19,22,23,26,42,44–47,49,51,56,91,92]. Therefore, it is preferable to avoid antibodies whenever possible to minimize the risk of locking the transporter in a nonphysiological conformation.…”

Section: Cryo‐em In Abc‐transporter Drug Discoverymentioning

confidence: 99%

“…As such, cryo-EM enabled the analysis of ABC transporters that defied crystallography, such as the cystic fibrosis transmembrane conductance regulator (CFTR) [6,[19][20][21][22][23] and ABCG2 [7,[24][25][26], also known as breast cancer resistance protein (BCRP). Moreover, the low sample amount requirements in cryo-EM provide the opportunity to study low-abundant, native, fragile, or flexible complexes [27][28][29][30][31][32][33][34], while the high tolerance to various hydrophobic environments [35][36][37][38][39][40][41] enables structure determination of ABC transporters not only in different detergents [5,6,28,29,[42][43][44][45][46][47][48][49][50][51][52], but also within a lipid environment [8,24,[53][54][55][56]. Additionally, cryo-EM can dissect confo...…”

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confidence: 99%

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Cryo‐EM of ABC transporters: an ice‐cold solution to everything?

Januliene

Moeller

2020

FEBS Letters

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High-resolution cryo-EM has revolutionized how we look at ABC transporters and membrane proteins in general. An ever-increasing number of software tools and faster processing now allow dissecting the molecular details of nanomachines at atomic precision. Considering the further benefits of significantly reduced sample demands and increased speed, cryo-EM will dominate the structure determination of membrane proteins in the near future without compromising on data quality or detail. Moreover, improved and new algorithms make it now possible to resolve the conformational spectrum of macromolecular machines under turnover conditions and to analyze heterogeneous samples at high-resolution. The future of cryo-EM is, therefore, bright, and the growing number of imaging facilities and groups active in this field will amplify this trend even further. Nevertheless, expectations have to be managed, as cryo-EM alone cannot provide an ultimate answer to all scientific questions. In this review, we discuss the capabilities and limitations of cryo-EM together with possible solutions for studies of ABC transporters.

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Zeitaufgelöste Mn²⁺−NO‐ und NO−NO‐Abstandsmessungen zeigen regulierende Funktion der katalytischen Asymmetrie auf den alternierenden Zugang in einem ABC‐Transporter**

Tampé

Joseph

2023

Angewandte Chemie

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ATP‐binding cassette Transporter (ABC‐Transporter) transportieren unterschiedlichste Substrate über biologische Membranen. Der Transport erfolgt durch den Übergang zwischen einer nach innen gerichteten (IF) und einer nach außen gerichteten (OF) Konformation der Transmembrandomänen (TMD). Katalytisch asymmetrische Nukleotidbindestellen (NBS) sind in fast allen ABC‐Proteinunterfamilien vorhanden, ihre funktionelle Rolle ist jedoch noch nicht geklärt. Wir haben diese Frage mit Hilfe von gleichzeitigen NO−NO, Mn2+−NO und Mn2+−Mn2+ Abstandsmessungen mittels gepulster Doppel‐Elektron‐Elektron‐Resonanzspektroskopie von TmrAB zeitaufgelöst untersucht. Dieser Typ IV ABC‐Transporter durchläuft in Gegenwart von ATP einen reversiblen Übergang mit einem deutlich schnelleren Vorwärtsübergang (IF‐nach‐OF). Die katalytisch beeinträchtigte, degenerierte NBS bindet Mn2+−ATP stabil, während Mn2+ bevorzugt an der aktiven konsensus NBS freigesetzt wird. Die ATP‐Hydrolyse an der konsensus NBS beschleunigt den Rückwärtsübergang erheblich. Beide NBSs öffnen sich während jedes Konformationszyklus vollständig, und die degenerierte NBS könnte die Kinetik dieses Prozesses regulieren.

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Structure of the human lipid exporter ABCB4 in a lipid environment

Cited by 76 publications

References 92 publications

Structural and functional diversity calls for a new classification of ABC transporters

Structural and functional diversity calls for a new classification of ABC transporters

Cryo‐EM of ABC transporters: an ice‐cold solution to everything?

Zeitaufgelöste Mn²⁺−NO‐ und NO−NO‐Abstandsmessungen zeigen regulierende Funktion der katalytischen Asymmetrie auf den alternierenden Zugang in einem ABC‐Transporter**

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Structure of the human lipid exporter ABCB4 in a lipid environment

Cited by 76 publications

References 92 publications

Structural and functional diversity calls for a new classification of ABC transporters

Structural and functional diversity calls for a new classification of ABC transporters

Cryo‐EM of ABC transporters: an ice‐cold solution to everything?

Zeitaufgelöste Mn2+−NO‐ und NO−NO‐Abstandsmessungen zeigen regulierende Funktion der katalytischen Asymmetrie auf den alternierenden Zugang in einem ABC‐Transporter**

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Zeitaufgelöste Mn²⁺−NO‐ und NO−NO‐Abstandsmessungen zeigen regulierende Funktion der katalytischen Asymmetrie auf den alternierenden Zugang in einem ABC‐Transporter**