Sandbox 125
From Proteopedia
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=='''How does Kapβ2 release its cargo? '''== | =='''How does Kapβ2 release its cargo? '''== | ||
- | Ran is a GTP binding protein that is found in greater concentrations in the nucleus than in the cytoplasm. In the nucleus Ran Guanine Nucleotide Exchange Factor (ranGEF) is a protein that catalyzes the dissociation of GDP from Ran and subsequent phosphorylation. Ran-GTP undergoes conformational changes that allow it to have a greater affinity for Kapβ2 than Ran-GDP. These conformational changes occur in Ran between residues 30-47 and residues 65-80, and | + | Ran is a GTP binding protein that is found in greater concentrations in the nucleus than in the cytoplasm. In the nucleus Ran Guanine Nucleotide Exchange Factor (ranGEF) is a protein that catalyzes the dissociation of GDP from Ran and subsequent phosphorylation. Ran-GTP undergoes conformational changes that allow it to have a greater affinity for Kapβ2 than Ran-GDP. These conformational changes occur in Ran between residues 30-47 and residues 65-80. |
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+ | RanGTP has an overall positive charge allowing it to bind to the highly negative core of the N-terminal arch Kapβ2. There are two distinct regions of polar interaction between KapB2 and RanGTP. These regions of Kapβ2 are defined as the N Interface found within HR1-3, and the Central Interface found within HR6, HR7, 62-residue loop of HR8, HR13 and HR14. | ||
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+ | Polar interactions at the N Interface include Ser22, Arg31, Glu161, Asp 164 and Ser165 of KapB2, and Trp64, Val45, Arg110, and Arg106 of RanGTP. | ||
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+ | Polar interactions at the Central Interface include Asn271, Glu275, Glu278, Glu332, Glu333, Asp334, Arg336, His340, Glu363, Ile364, Asp366, Asp367, Ile370, Ser371, Trp373, Lys377, Asp639, Glu682 of KapB2 and Asn143, Lys141, Arg140, Asn154, Asn156, Lys159, Asp148, Tyr155, Lys127, Lys134, Lys132, Arg129, His139, Tyr 146, Gln145, Asn143, Arg140, and Lys127 of RanGTP. | ||
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+ | When RanGTP binds to Kapβ2 conformational changes occur within the N-terminal arch and within a long (62 residue) loop of HEAT repeat 8. It is the changes in the 62-residue loop (residues 311-373) that is important in the dissociation of the NLS. It is thought that the 62- residue loop binds into the NLS binding site thus releasing the NLS. | ||
- | RanGTP has an overall positive charge allowing it to bind to the highly negative core of the N-terminal arch Kapβ2. There are two distinct regions of polar interaction between KapB2 and RanGTP. These regions of Kapβ2 are defined as the N Interface found within HR1-3, and the Central Interface found within HR6, HR7, 62-residue loop of HR8, HR13 and HR14. The following chart includes the polar interactions of KapB2 with RanGTP at both the N Interface and Central Interface. | ||
</StructureSection> | </StructureSection> |
Revision as of 22:21, 2 January 2014
Introduction
Karyopherin Beta 2 (Kapβ2) is an importin that transports various cargo proteins into the nucleus through interactions with nucleoporins, which are proteins of the nuclear pore complex (NPC). One might overlook the significance of this protein but it actually plays a crucial role in the human body by mediating transport of RNA-binding proteins involved in Transcription and RNA Processing, RNA transport and translation. The structure of Kapβ2 is composed of 20 antiparallel helices called HEAT repeats. These HEAT repeats contribute to Kapβ2’s large superhelical shape. The protein is shown to form two arches: one at the N-terminal and the other at the C-terminal. Through recognition of a nuclear localization signal (NLS) located on its cargo, Kapβ2 binds to its cargo via its C-terminal arch. Release of the cargo is mediated by RanGTP, which once bound, leads to a large movement of the 62-residue heat repeat 8 loop into the C-terminal arch. This conformational change results in the dissociation of the cargo as the b2 loop binds the NLS binding site.
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