The global impact of hybrid electric vehicles (HEVs) is exponentially rising as it is an emission-free and reliable alternative to fossil fuel-based vehicles that cause enormous negative impacts on the socioeconomic and environmental sectors. Fuel cell hybrid electric vehicles (FCHEV) have been widely considered in the latest research as an energy-efficient, environmentally friendly, and longer-range green transportation alternative. The performance of these FCHEVs, however, is primarily dependent upon the optimal selection of Energy Management Strategies (EMSs) adopted for optimum power split and energy resource management. This research reviews the latest EMS techniques presented in the literature and highlights their working principle, operation, and impact on the FCHEV performance and reliability. This research also highlights the challenges associated with the globalization of FCHEVs and recommends future work and research directions essential for optimal FCHEV performance and commercialization.
The Mycobacterium tuberculosis genome harbours nine toxin-antitoxin (TA) systems of the mazEF family. These consist of two proteins, a toxin and an antitoxin, encoded in an operon. While the toxin has a conserved fold, the antitoxins are structurally diverse and the toxin binding region is typically intrinsically disordered before binding. We describe high throughput methodology for accurate mapping of interfacial residues and apply it to three MazEF complexes. The method involves screening one partner protein against a panel of chemically masked single cysteine mutants of its interacting partner, displayed on the surface of yeast cells. Such libraries have much lower diversity than those generated by saturation mutagenesis, simplifying library generation and data analysis. Further, because of the steric bulk of the masking reagent, labeling of virtually all exposed epitope residues should result in loss of binding, and buried residues are inaccessible to the labeling reagent. The binding residues are deciphered by probing the loss of binding to the labeled cognate partner by flow cytometry. Using this methodology, we have identified the interfacial residues for MazEF3, MazEF6 and MazEF9 TA systems of M. tuberculosis. In the case of MazEF9, where a crystal structure was available, there was excellent agreement between our predictions and the crystal structure, superior to those with AlphaFold2. We also report detailed biophysical characterization of the MazEF3 and MazEF9 TA systems and measured the relative affinities between cognate and non-cognate toxin–antitoxin partners in order to probe possible cross-talk between these systems.
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