Half Sphere exposure (HSE) is a protein solvent exposure measure that was first introduced by . Like all solvent exposure measures it measures how buried amino acid residues are in a protein. It is found by counting the number of amino acid neighbors within two half spheres of chosen radius around the amino acid. The calculation of HSE is found by dividing a contact number (CN) sphere in two halves by the plane perpendicular to the Cò-Cñ vector. This simple division of the CN sphere results in two strikingly different measures, HSE-up and HSE-down. HSE-up is defined as the number of Cñ atoms in the upper half (containing the pseudo-Cò atom) and analogously HSE-down is defined as the number of Cñ atoms in the opposite sphere.
If only Cñ atoms are available (as is the case for many simplified representations of protein structure), a related measure, called HSEñ, can be used. HSEñ uses a pseudo-Cò instead of the real Cò atom for its calculation. The position of this pseudo-Cò atom (pCò) is derived from the positions of preceding Cñ<sup>âÂÂ1</sup> and the following Cñ<sup>+1</sup>. The Cñ-pCò vector is calculated by adding the Cñ<sup>âÂÂ1</sup>-Cñ<sup>0</sup> and Cñ<sup>+1</sup>-Cñ<sup>0</sup> vectors.
HSE is used in predicting discontinuous B-cell epitopes. Song et al. have developed an online webserver termed HSEpred to predict half-sphere exposure from protein primary sequences. HSEpred server can achieve the correlation coefficients of 0.72 and 0.68 between the predicted and observed HSE-up and HSE-down measures, respectively, when evaluated on a well-prepared non-homologous protein structure dataset. Moreover, residue contact number (CN) can also be accurately predicted by HSEpred webserver using the summation of the predicted HSE-up and HSE-down values, which has further enlarged the application of this new solvent exposure measure.
Recently, Heffernan et al. has developed the most accurate predictor for both HSEñ and HSEò based on a big dataset by using multiple-step iterative deep neural-network learning. The predicted HSEa shows a higher correlation coefficient to the stability change by residue mutants than predicted HSEò and ASA. The results, together with its easy Ca-atom-based calculation, highlight the potential usefulness of predicted HSEa for protein structure prediction and refinement as well as function prediction.