ABSTRACT
Loss-of-function mutations of the protein kinase PERK (EIF2AK3) in humans and mice cause permanent neonatal diabetes and severe proinsulin aggregation in the endoplasmic reticulum (ER), highlighting the essential role of PERK in insulin production in pancreatic ß cells. As PERK is generally known as a translational regulator of the unfolded protein response (UPR), the underlying cause of these ß cell defects has often been attributed to derepression of proinsulin synthesis, resulting in proinsulin overload in the ER. Using high-resolution imaging and standard protein fractionation and immunological methods we have examined the PERK-dependent phenotype more closely. We found that whereas proinsulin aggregation requires new protein synthesis, global protein and proinsulin synthesis are down-regulated in PERK-inhibited cells, strongly arguing against proinsulin overproduction being the root cause of their aberrant ER phenotype. Furthermore, we show that PERK regulates proinsulin proteostasis by modulating ER chaperones, including BiP and ERp72. Transgenic overexpression of BiP and BiP knockdown (KD) both promoted proinsulin aggregation, whereas ERp72 overexpression and knockdown rescued it. These findings underscore the importance of ER chaperones working in concert to achieve control of insulin production and identify a role for PERK in maintaining a functional balance among these chaperones.
Subject(s)
Proinsulin/metabolism , eIF-2 Kinase/metabolism , Animals , Diabetes Mellitus/metabolism , Endoplasmic Reticulum/physiology , Glucose/metabolism , Humans , Insulin/metabolism , Insulin-Secreting Cells/metabolism , Mice , Mice, Knockout , Molecular Chaperones/metabolism , Proinsulin/genetics , Protein Biosynthesis/drug effects , Unfolded Protein Response/drug effects , eIF-2 Kinase/geneticsABSTRACT
Mg-S batteries are attractive for next-generation energy storage because of their high theoretical capacity and low cost. The foremost challenge in Mg-S batteries is designing electrolytes that support reversible electrochemistry at both electrodes. Here, we target a solution-mediated reduction pathway for the S8 cathode by tailoring the electrolyte solvent. Varying the solvent in Mg-based systems is complicated because of the active nature of the solvent in solvating Mg2+ and the complex dynamics of electrolyte-Mg interfaces. To understand the effect of the solvent on the S8 reduction processes in the Mg-S cell, the magnesium-aluminum chloride complex (MACC) electrolyte was prepared in different ethereal solvents. Reversible Mg electrodeposition is demonstrated in the MACC electrolyte in several solvent systems. The electrodeposition overpotentials and current densities are found to vary with the solvent, suggesting that the solvent plays a noninnocent role in the electrochemical processes at the Mg interface. Mg-S cells are prepared with the electrolytes to understand how the solvent affects the reduction of S8. A reductive wave is present in all linear-sweep voltammograms, and the peak potential varies with the solvent. The peak potential is approximately 0.8 V versus Mg/Mg2+, lower than the expected reduction potential of 1.7 V. We rule out passivation of the Mg anode as the cause for the low voltage peak potential, making processes at the S8 cathode the likely culprit. The ability to oxidize MgS with the MACC electrolyte is also examined, and we find that the oxidation current can be attributed to side reactions at the C-electrolyte interface.
ABSTRACT
Mg-based batteries are an attractive next-generation energy storage chemistry due to the high natural abundance and inexpensive cost of Mg, along with the high theoretical energy density compared to that of conventional Li-ion chemistry. The greater energy density is predicated on a Mg metal anode, and pathways to achieving reversible Mg electrodeposition and stripping are reliant on the development of Mg electrolytes. Although Mg electrolyte chemistry has advanced significantly from the reactive Grignards of the 1920s to the carboranes of this decade, there remains significant challenges in correlating the Mg metal anode electrochemistry with the composition of the electrolyte salts as a result of the complicated interface of Mg metal and the electrolyte. To probe the effect of the interface on Mg electrodeposition, we turn to an electrolyte with a known solution-phase composition: the magnesium aluminum chloride complex (MACC) electrolyte. The MACC electrolyte requires electrolytic conditioning to support reversible Mg electrodeposition and stripping. Here, we show that a small concentration (2-5 mM) of Mg(HMDS)2 with respect to the MACC electrolyte salts suppresses Al3+ deposition and promotes reversible Mg electrodeposition and stripping in the first cycle. The significant effect of a small concentration of additive is attributed to changes to the electrode interface. The impact of the Mg interface on the observed electrochemical performance is discussed.