Mechanism of RanGTP priming H2A-H2B release from Kap114 in an atypical RanGTP•Kap114•H2A-H2B complex

Jiou, Jenny; Shaffer, Joy M.; Bernades, Natalia E.; Fung, Ho Yee Joyce; Kikumoto Dias, Juliana; D’Arcy, Sheena; Chook, Yuh Min

doi:10.1073/pnas.2301199120

Cited by 2 publications

(14 citation statements)

References 51 publications

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“…In intact nuclei from human osteosarcoma U2OS cells, Ran was cross-linked to histones H2B, H3, and H4 . Additionally, Ran•GTP was found to form a complex with H2A-H2B and the histone chaperone importin 9 (as well as its yeast homologue Kap114) during nucleosome assembly. , In these ternary complexes, Ran•GTP modulates importin-histone interactions and makes transient contacts with α3 and αC of H2A. The complexation leads to a conformational change in importin 9/Kap114 that promotes the release of H2A-H2B into the assembling nucleosome.…”

Section: Resultsmentioning

confidence: 99%

“…The complexation leads to a conformational change in importin 9/Kap114 that promotes the release of H2A-H2B into the assembling nucleosome. As importin-9 binds to H2A-H2B via a mechanism also involving arginine interactions with the acidic patch as well as to Ran, , it is conceivable that, in the vicinity of chromatin, a high concentration of RCC1 may result in competition between importins and RCC1 for binding to both H2A-H2B and Ran. The Ran-nucleosome interactions mentioned above are not observed in our structure, which features Ran in its (mostly) nucleotide-free state (see below).…”

Section: Resultsmentioning

confidence: 99%

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Cryo-EM of the Nucleosome Core Particle Bound to Ran-RCC1 Reveals a Dynamic Complex

Huang,

Rubinstein,

Kay

2024

Biochemistry

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Ras-related nuclear protein (Ran) is a member of the Ras superfamily of small guanosine triphosphatases (GTPases) and a regulator of multiple cellular processes. In healthy cells, the GTP-bound form of Ran is concentrated at chromatin, creating a Ran•GTP gradient that provides the driving force for nucleocytoplasmic transport, mitotic spindle assembly, and nuclear envelope formation. The Ran•GTP gradient is maintained by the regulator of chromatin condensation 1 (RCC1), a guanine nucleotide exchange factor that accelerates GDP/GTP exchange in Ran. RCC1 interacts with nucleosomes, which are the fundamental repeating units of eukaryotic chromatin. Here, we present a cryo-EM analysis of a trimeric complex composed of the nucleosome core particle (NCP), RCC1, and Ran. While the contacts between RCC1 and Ran in the complex are preserved compared with a previously determined structure of RCC1-Ran, our study reveals that RCC1 and Ran interact dynamically with the NCP and undergo rocking motions on the nucleosome surface. Furthermore, the switch 1 region of Ran, which plays an important role in mediating conformational changes associated with the substitution of GDP and GTP nucleotides in Ras family members, appears to undergo disorder–order transitions and forms transient contacts with the C-terminal helix of histone H2B. Nucleotide exchange assays performed in the presence and absence of NCPs are not consistent with an active role for nucleosomes in nucleotide exchange, at least in vitro. Instead, the nucleosome stabilizes RCC1 and serves as a hub that concentrates RCC1 and Ran to promote efficient Ran•GDP to Ran•GTP conversion.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Cryo-EM of the Nucleosome Core Particle Bound to Ran-RCC1 Reveals a Dynamic Complex

Huang,

Rubinstein,

Kay

2024

Biochemistry

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“…Biochemical and structural studies of binary Kap114-H2A-H2B and Nap1 2 -H2A-H2B interactions, and pull-down studies of Kap114 and Nap1 from yeast lysates have been reported (13, 22, 36, 41). First, we confirmed the previous findings using analytical ultracentrifugation (AUC), size exclusion chromatography multi-angle light scattering (SEC-MALS) and pull-down binding assays with recombinant Kap114, Nap1 and H2A-H2B (SI Appendix, Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The superhelical Kap114 wraps around the H2A-H2B histone-fold domain (Fig. 1B), occluding the histone’s DNA-binding surfaces and thus also acting as a histone chaperone (40, 41). The Kap114•H2A-H2B complex is unusual in its interactions with the GTPase Ran GTP .…”

Section: Introductionmentioning

confidence: 99%

“…The Kap114•H2A-H2B complex is unusual in its interactions with the GTPase Ran GTP . Most importin•cargo complexes are dissociated by Ran GTP but Kap114•H2A-H2B binds Ran GTP to form a stable Ran GTP •Kap114•H2A-H2B complex, which alters interactions between Kap114 and H2A-H2B, and facilitates histone transfer to other nuclear chaperones or to the assembling nucleosome (41).…”

Section: Introductionmentioning

confidence: 99%

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Nap1 and Kap114 co-chaperone H2A-H2B and facilitate targeted histone release in the nucleus

Jiou

Fung

Chook

2023

Preprint

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Histones are synthesized and processed in the cytoplasm and then transported into the nucleus for assembly into nucleosomes. H2A-H2B is imported into the S. cerevisiae nucleus by the importin Kap114, which also imports the most prominent H2A-H2B chaperone, Nap1. We understand how Kap114 recognizes H2A-H2B for nuclear import, but little is known about how it recognizes Nap1. Furthermore, the ternary complex of Nap1, H2A-H2B and Kap114 was previously detected in both the cytosol and the nucleus, but its role in nuclear import is unclear. Here, we present biophysical analysis of interactions between Nap1, H2A-H2B, Kap114 and RanGTP, and cryo-electron microscopy structures of ternary Kap114, Nap1 and H2A-H2B complexes. Kap114 binds Nap1 very weakly, but H2A-H2B enhances Kap114-Nap1 interaction to form a ternary Kap114/Nap1/H2A-H2B complex that is stable in the absence and presence of RanGTP. Cryogenic electron microscopy structures reveal two distinct ternary Kap114/Nap1/H2A-H2B complexes: a 3.2 Å resolution structure of Nap1 bound to H2A-H2B-bound Kap114 where Nap1 does not contact H2A-H2B, and a 3.5 Å resolution structure of H2A-H2B sandwiched between Nap1 and Kap114. Collectively, these results lead to a mechanistic model of how Nap1·H2A-H2B encounters Kap114 in the cytoplasm and how both H2A-H2B and Nap1 are chaperoned and co-imported by Kap114 into the nucleus. The model also suggests how RanGTP-binding stabilizes a quaternary RanGTP/Kap114/Nap1/H2A-H2B complex that facilitates hand-off of H2A-H2B from Kap114 to Nap1, the assembling nucleosome or other nuclear chaperone.

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Mechanism of RanGTP priming H2A-H2B release from Kap114 in an atypical RanGTP•Kap114•H2A-H2B complex

Cited by 2 publications

References 51 publications

Cryo-EM of the Nucleosome Core Particle Bound to Ran-RCC1 Reveals a Dynamic Complex

Cryo-EM of the Nucleosome Core Particle Bound to Ran-RCC1 Reveals a Dynamic Complex

Nap1 and Kap114 co-chaperone H2A-H2B and facilitate targeted histone release in the nucleus

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