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Elevated temperatures impair pollen performance and reproductive success, resulting in lower crop yields. The tomato (Solanum lycopersicum) anthocyanin reduced (are) mutant harbors a mutation in FLAVANONE 3-HYDROXYLASE (F3H), resulting in impaired flavonol antioxidant biosynthesis. The are mutant has reduced pollen performance and seed set relative to the VF36 parental line, phenotypes that are accentuated at elevated temperatures. Transformation of are with the wild-type F3H gene, or chemical complementation with flavonols, prevented temperature-dependent reactive oxygen species (ROS) accumulation in pollen and restored the reduced viability, germination, and tube elongation of are to VF36 levels. Overexpression of F3H in VF36 prevented temperature-driven ROS increases and impaired pollen performance, revealing that flavonol biosynthesis promotes thermotolerance. Although stigmas of are had reduced flavonol and elevated ROS levels, the growth of are pollen tubes was similarly impaired in both are and VF36 pistils. RNA-seq was performed at optimal and stress temperatures in are, VF36, and the F3H overexpression line at multiple timepoints across pollen tube elongation. The number of differentially expressed genes increased over time under elevated temperatures in all genotypes, with the greatest number in are. These findings suggest potential agricultural interventions to combat the negative effects of heat-induced ROS in pollen that lead to reproductive failure. 

While many real-world programs are shipped with configurations to enable/disable functionalities, fuzzers have mostly been applied to test single configurations of these programs. In this work, we first conduct an empirical study to understand how program configurations affect fuzzing performance. We find that limiting a campaign to a single configuration can result in failing to cover a significant amount of code. We also observe that different program configurations contribute differing amounts of code coverage, challenging the idea that each one can be efficiently fuzzed individually. Motivated by these two observations, we propose ConfigFuzz , which can fuzz configurations along with normal inputs. ConfigFuzz transforms the target program to encode its program options within part of the fuzzable input, so existing fuzzers’ mutation operators can be reused to fuzz program configurations. We instantiate ConfigFuzz on six configurable, common fuzzing targets, and integrate their executions in FuzzBench. In our evaluation, ConfigFuzz outperforms two baseline fuzzers in four targets, while the results are mixed in the other targets due to program size and configuration space. We also analyze the options fuzzed by ConfigFuzz and how they affect the performance. 

2LiX-GaF₃(X = Cl, Br, I) electrolytes offer favorable features for solid-state batteries: mechanical pliability and high conductivities. However, understanding the origin of fast ion transport in 2LiX-GaF₃has been challenging. The ionic conductivity order of 2LiCl-GaF₃(3.20 mS/cm) > 2LiBr-GaF₃(0.84 mS/cm) > 2LiI-GaF₃(0.03 mS/cm) contradicts binary LiCl (10⁻¹²S/cm) < LiBr (10⁻¹⁰S/cm) < LiI (10⁻⁷S/cm). Using multinuclear⁷Li,⁷¹Ga,¹⁹F solid-state nuclear magnetic resonance and density functional theory simulations, we found that Ga(F,X)_npolyanions boost Li⁺-ion transport by weakening Li⁺-X⁻interactions via charge clustering. In 2LiBr-GaF₃and 2LiI-GaF₃, Ga-X coordination is reduced with decreased F participation, compared to 2LiCl-GaF₃. These insights will inform electrolyte design based on charge clustering, applicable to various ion conductors. This strategy could prove effective for producing highly conductive multivalent cation conductors such as Ca²⁺and Mg²⁺, as charge clustering of carboxylates in proteins is found to decrease their binding to Ca²⁺and Mg²⁺. 

ABSTRACT The kidney filters nutrient waste and bodily fluids from the bloodstream, in addition to secondary functions of metabolism and hormone secretion, requiring an astonishing amount of energy to maintain its functions. In kidney cells, mitochondria produce adenosine triphosphate (ATP) and help maintain kidney function. Due to aging, the efficiency of kidney functions begins to decrease. Dysfunction in mitochondria and cristae, the inner folds of mitochondria, is a hallmark of aging. Therefore, age-related kidney function decline could be due to changes in mitochondrial ultrastructure, increased reactive oxygen species (ROS), and subsequent alterations in metabolism and lipid composition. We sought to understand if there is altered mitochondrial ultrastructure, as marked by 3D morphological changes, across time in tubular kidney cells. Serial block facing-scanning electron microscope (SBF-SEM) and manual segmentation using the Amira software were used to visualize murine kidney samples during the aging process at 3 months (young) and 2 years (old). We found that 2-year mitochondria are more fragmented, compared to the 3-month, with many uniquely shaped mitochondria observed across aging, concomitant with shifts in ROS, metabolomics, and lipid homeostasis. Furthermore, we show that the mitochondrial contact site and cristae organizing system (MICOS) complex is impaired in the kidney due to aging. Disruption of the MICOS complex shows altered mitochondrial calcium uptake and calcium retention capacity, as well as generation of oxidative stress. We found significant, detrimental structural changes to aged kidney tubule mitochondria suggesting a potential mechanism underlying why kidney diseases occur more readily with age. We hypothesize that disruption in the MICOS complex further exacerbates mitochondrial dysfunction, creating a vicious cycle of mitochondrial degradation and oxidative stress, thus impacting kidney health. Translational StatementDue to aging, the efficiency of kidney functions begins to decrease and the risk of kidney diseases may increase, but specific regulators of mitochondrial age-related changes are poorly explained. This study demonstrates the MICOS complex may be a target for mitigating age-related changes in mitochondria. The MICOS complex can be associated with oxidative stress and calcium dysregulation, which also arise in many kidney pathologies. Graphical AbstractKidney aging causes a decline in the MICOS complex, concomitant with metabolic, lipidomic, and mitochondrial structural alterations.