Efficient Exploitation of Numerical Quadrature with Distance-Dependent Integral Screening in Explicitly Correlated F12 Theory: Linear Scaling Evaluation of the Most Expensive RI-MP2-F12 Term.

We present a linear scaling atomic orbital based algorithm for the computation of the most expensive exchange-type RI-MP2-F12 term by employing numerical quadrature in combination with CABS-RI to avoid six-center-three-electron integrals. Furthermore, a robust distance-dependent integral screening scheme, based on integral partition bounds [Thompson, T. H.; Ochsenfeld, C. J. Chem. Phys. 2019, 150, 044101], is used to drastically reduce the number of the required three-center-one-electron integrals substantially. The accuracy of our numerical quadrature/CABS-RI approach and the corresponding integral screening is thoroughly assessed for interaction and isomerization energies across a variety of numerical integration grids. Our method outperforms the standard density fitting/CABS-RI approach with errors below 1 µEh even for small grid sizes and moderate screening thresholds. The choice of the grid size and screening threshold allows us to tailor our ansatz to a desired accuracy and computational efficiency. We showcase the approach's effectiveness for the chemically relevant system valinomycin, employing a triple-ζ F12 basis set combination (C54H90N6O18, 5757 AO basis functions, 10,266 CABS basis functions, 735,783 grid points). In this context, our ansatz achieves higher accuracy combined with a 135× speedup compared to the classical density fitting based variant, requiring notably less computation time than the corresponding RI-MP2 calculation. Additionally, we demonstrate near-linear scaling through calculations on linear alkanes. We achieved an 817-fold acceleration for C80H162 and an extrapolated 28,765-fold acceleration for C200H402, resulting in a substantially reduced computational time for the latter─from 229 days to just 11.5 min. Our ansatz may also be adapted to the remaining MP2-F12 terms, which will be the subject of future work.

Highly Efficient and Accurate Computation of Multiple Orbital Spaces Spanning Fock Matrix Elements on Central and Graphics Processing Units for Application in F12 Theory.

We employ our recently published highly efficient seminumerical exchange (sn-LinK) [Laqua, H.; Thompson, T. H.; Kussmann, J.; Ochsenfeld, C. J. Chem. Theory Comput. 2020, 16, 1456-1468] and integral-direct resolution of the identity Coulomb (RI-J) [Kussmann, J.; Laqua, H.; Ochsenfeld, C. J. Chem. Theory Comput. 2021, 17, 1512-1521] methods to significantly accelerate the computation of the demanding multiple orbital spaces spanning Fock matrix elements present in R12/F12 theory on central and graphics processing units. The errors introduced by RI-J and sn-LinK into the RI-MP2-F12 energy are thoroughly assessed for a variety of basis sets and integration grids. We find that these numerical errors are always below "chemical accuracy" (∼1 mH) even for the coarsest settings and can easily be reduced below 1 µH by employing only moderately large integration grids and RI-J basis sets. Since the number of basis functions of the multiple orbital spaces is notably larger compared with conventional Hartree-Fock theory, the efficiency gains from the superior basis scaling of RI-J and sn-LinK (O(Nbas2) instead of O(Nbas4) for both) are even more significant, with maximum speedup factors of 37 000 for RI-J and 4500 for sn-LinK. In total, the multiple orbital spaces spanning Fock matrix evaluation of the largest tested structure using a triple-ζ F12 basis set (5058 AO basis functions, 9267 CABS basis functions) is accelerated over 1575× using CPUs and over 4155× employing GPUs.

Identification of the subtype-selective Sirt5 inhibitor balsalazide through systematic SAR analysis and rationalization via theoretical investigations.

We report here an extensive structure-activity relationship study of balsalazide, which was previously identified in a high-throughput screening as an inhibitor of Sirt5. To get a closer understanding why this compound is able to inhibit Sirt5, we initially performed docking experiments comparing the binding mode of a succinylated peptide as the natural substrate and balsalazide with Sirt5 in the presence of NAD+. Based on the evidence gathered here, we designed and synthesized 13 analogues of balsalazide, in which single functional groups were either deleted or slightly altered to investigate which of them are mandatory for high inhibitory activity. Our study confirms that balsalazide with all its given functional groups is an inhibitor of Sirt5 in the low micromolar concentration range and structural modifications presented in this study did not increase potency. While changes on the N-aroyl-ß-alanine side chain eliminated potency, the introduction of a truncated salicylic acid part minimally altered potency. Calculations of the associated reaction paths showed that the inhibition potency is very likely dominated by the stability of the inhibitor-enzyme complex and not the type of inhibition (covalent vs. non-covalent). Further in-vitro characterization in a trypsin coupled assay determined that the tested inhibitors showed no competition towards NAD+ or the synthetic substrate analogue ZKsA. In addition, investigations for subtype selectivity revealed that balsalazide is a subtype-selective Sirt5 inhibitor, and our initial SAR and docking studies pave the way for further optimization.

Development of an Advanced Force Field for Water Using Variational Energy Decomposition Analysis.

Given the piecewise approach to modeling intermolecular interactions for force fields, they can be difficult to parametrize since they are fit to data like total energies that only indirectly connect to their separable functional forms. Furthermore, by neglecting certain types of molecular interactions such as charge penetration and charge transfer, most classical force fields must rely on, but do not always demonstrate, how cancellation of errors occurs among the remaining molecular interactions accounted for such as exchange repulsion, electrostatics, and polarization. In this work we present the first generation of the (many-body) MB-UCB force field that explicitly accounts for the decomposed molecular interactions commensurate with a variational energy decomposition analysis, including charge transfer, with force field design choices that reduce the computational expense of the MB-UCB potential while remaining accurate. We optimize parameters using only a single water molecule and water cluster data up through pentamers, with no fitting to condensed phase data, and we demonstrate that high accuracy is maintained when the force field is subsequently validated against conformational energies of larger water cluster data sets, radial distribution functions of the liquid phase, and the temperature dependence of thermodynamic and transport water properties. We conclude that MB-UCB is comparable in performance to MB-Pol but is less expensive and more transferable by eliminating the need to represent short-ranged interactions through large parameter fits to high order polynomials.