Abstract
The two forms of transthyretin differing slightly in the tertiary structure, despite the presence of five mutations, show radically different properties in terms of susceptibility to the amyloid transformation process. These two forms of transthyretin are the object of analysis. The search for the sources of these differences was carried out by means of a comparative analysis of the structure of these molecules in their native and early intermediate stage forms in the folding process. The criterion for assessing the degree of similarity and differences is the status of the hydrophobic core. The comparison of the level of arrangement of the hydrophobic core and its initial stages is possible thanks to the application of divergence entropy for the early intermediate stage and for the final forms. It was shown that the minimal differences observed in the structure of the hydrophobic core of the forms available in PDB, turned out to be significantly different in the early stage (ES) structure in folding process. The determined values of divergence entropy for both ES forms indicate the presence of the seed of hydrophobic core only in the form resistant to amyloid transformation. In the form of aggressively undergoing amyloid transformation, the structure lacking such a seed is revealed, being a stretched one with a high content of β-type structure. In the discussed case, the active presence of water in the structural transformation of proteins expressed in the fuzzy oil drop model (FOD) is of decisive importance for the generation of the final protein structure. It has been shown that the resistant form tends to generate a centric hydrophobic core with the possibility of creating a globular structure, i.e., a spherical micelle-like form. The aggressively transforming form reveals in the structure of its early intermediate, a tendency to form the ribbon-like micelle as observed in amyloid.
Highlights
Since the identification of aggregates causing pathological phenomena—amyloids—which are the effect of so-called misfolding, the perception of the process of protein folding has changed [1]
Mutations at positions 87 and 110 introduce negligible changes, the focus was on the section 43–58, which based on the fuzzy oil drop model contribute to the potential amyloid transformation
Structural characteristics of transthyretin based on the quantification of the presence of hydrophobic core both in the form of an early and late intermediates is possible thanks to the use of divergence entropy
Summary
Since the identification of aggregates causing pathological phenomena—amyloids—. Which are the effect of so-called misfolding, the perception of the process of protein folding has changed [1]. The dogma assuming determination of 3D structure by amino acids sequence [2] become questioned in context of misfolding phenomenon especially for amyloid transformation which takes place without any chemical modification of the original protein molecule Next to “folding” the phenomenon of “misfolding” became the object of analysis [1]. The importance of transthyretin is significant due to the pathological phenomena caused by the structural changes of this protein leading to the generation of amyloid deposits. The role of the quaternary structure turns out to be critical for this phenomenon [10,11,12,13,14].
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