2. For antisymmetric excitations, it is possible to obtain , . Respective lengths are as follows: In
this type of excitation, one of the peptide chains AZD6738 manufacturer does not change (here, it is a chain with the number 2), and two others are reduced up to the value . Such asymmetry is enough for the alpha-helix to take a form of the segment of torus instead of cylinder (Figure 3). Application of the simple geometric considerations gives for the radius of curvature R k and angle φ: and for displacement Δ, it is possible to get such estimation: (16) Taking into account the numerical values β ~ 10−1, R 0 = 5.4 Å, and d α = 4.56 Å in (16) gives . For the typical number of turns in many enzymes and membrane squirrel (N c > 10), displacement Alvespimycin will have an order Δ > 2 Å. This is consistent with the observed values [11]. 3. For asymmetrical excitation, the following values are implemented: , . The corresponding lengths of peptide chains equal The 4SC-202 datasheet nature of the distribution of deformation along the peptide chain for this type of excitation is similar to that of the antisymmetric excitation. The only difference is that the chain, which in the previous case has not changed at all, now has shortening stronger than
the other two. It is possible to estimate displacement for this case too: Here, Δ is the displacement for antisymmetric excitations, which is determined by Equation 16. Unlike displacement Δ, displacement Inositol monophosphatase 1 Δ(н) ‘directed’ to the opposite side. Executing numerical estimates, it is possible to set that Δ(н) > Δ, if the number of turns in the alpha-helix N c ≤ 14, but at N c > 14, we will have Δ(н) < Δ accordingly.
Consequently, asymmetrical excitations demonstrate two very interesting features. First, it has the lowest energy and at diminishment of the number of turns N c , it falls down yet more. Second, a conformational response for this type of excitation is the biggest for N c ≤ 14. This is typical for enzymatic proteins only. Figure 3 Explanation to estimation of displacement Δ of free (here upper) end of alpha-helix for antisymmetric excitations. Conclusions The general methods [7, 15–17] of description of the excited states of the condensed environments were applied to the alpha-helix region of a protein molecule. The alpha-helix is considered as a nanotube, and excitations of the environment are described as quasiparticles. It is shown that three different types of excitation exist, and each of them is probably used by three different types of protein. The symmetrical type of excitation is used for muscle proteins, the antisymmetric type of excitation is used for membrane proteins, and the asymmetric type of excitation is used for enzymatic proteins. It is possible that some excitations of asymmetrical type exist, which are also used by enzymes. The estimations were done for displacements of the free end of the alpha-helix. The obtained displacements are in agreement with experimental data.