AI Article Synopsis
- Two proteins from the β-grasp superfamily, specifically the B1-domain of protein G (GB1) and small archaeal modifier protein 1 (SAMP1), were studied to understand what makes their structures stable.
- Both proteins have a similar structure with two β-hairpins and a central α-helix, but their stability relies on different regions—GB1 is most stable at the C-terminal hairpin, while SAMP1 is more stable at the N-terminal hairpin.
- The findings suggest that the number and location of hydrophobic interactions play a crucial role in their stability, allowing these proteins to remain adaptable and flexible due to their symmetrical folding.
Article Abstract
Two proteins within the β-grasp superfamily, the B1-domain of protein G and the small archaeal modifier protein 1, were investigated to elucidate the key determinants of structural stability at the level of individual interactions. These symmetrical proteins both contain two β-hairpins which form a sheet flanked by a central α-helix. They were subjected to high temperature molecular dynamics simulations and the detailed behavior of each long-range interaction was characterized. The results revealed that in GB1 the most stable region was the C-terminal hairpin and in SAMP1 it was the opposite, the N-terminal hairpin. Experimental results for GB1 support this finding. In conclusion, it appears that the difference in the location and number of hydrophobic interactions dictate the differential stability which is accommodated due to structural symmetry of the β-grasp fold. Thus, the hairpins are interchangeable and in nature this lends itself to adaptability and flexibility.
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| http://dx.doi.org/10.1002/jcc.26477 | DOI Listing |
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