Comprehensive understanding of glioblastoma molecular phenotypes: classification, characteristics, and transition.

Among central nervous system-associated malignancies, glioblastoma (GBM) is the most common and has the highest mortality rate. The high heterogeneity of GBM cell types and the complex tumor microenvironment frequently lead to tumor recurrence and sudden relapse in patients treated with temozolomide. In precision medicine, research on GBM treatment is increasingly focusing on molecular subtyping to precisely characterize the cellular and molecular heterogeneity, as well as the refractory nature of GBM toward therapy. Deep understanding of the different molecular expression patterns of GBM subtypes is critical. Researchers have recently proposed tetra fractional or tripartite methods for detecting GBM molecular subtypes. The various molecular subtypes of GBM show significant differences in gene expression patterns and biological behaviors. These subtypes also exhibit high plasticity in their regulatory pathways, oncogene expression, tumor microenvironment alterations, and differential responses to standard therapy. Herein, we summarize the current molecular typing scheme of GBM and the major molecular/genetic characteristics of each subtype. Furthermore, we review the mesenchymal transition mechanisms of GBM under various regulators.

Effect of Heat Treatment on the Microstructure and Mechanical Properties of the Al0.6CoCrFeNi High-Entropy Alloy.

The effect of heat treatment on the microstructure and tensile properties of an as-cast Al0.6CoCrFeNi high-entropy alloy (HEA) was investigated in this paper. The results show that the as-cast Al0.6CoCrFeNi HEA presents a typical FCC dendrite morphology with the interdendritic region consisting of BCC/B2 structure and heat treatment can strongly affect the microstructure and mechanical properties of HEA. Microstructure analysis revealed the precipitation of a nano-sized L12 phase in the FCC dendrite and the formation of the FCC and σ phases in the interdendritic region after annealing at 700 °C. The coarse B2 phase was directly precipitated from the FCC dendrite in the 900 °C-annealed sample, with the coexistence of the B2, FCC, and σ phases in the interdendritic region. Then, the interdendritic region converted to a B2 and FCC dual-phase structure caused by the re-decomposition of the σ phase after annealing at 1100 °C. The tensile test results show that the 700 °C-annealed HEA presents the most significant strengthening effect, with increments of corresponding yield strength being about 107%, which can be attributed to the numerous nano-sized L12 precipitates in the FCC dendrite. The mechanical properties of 1100 °C-annealed alloy revert to a level close to that of the as-cast alloy, which can be attributed to the coarsening mechanism of B2 precipitates and the formation of a soft FCC phase in the interdendritic region. The observed variation in mechanical properties during heat treatment follows the traditional trade-off relationship between strength and plasticity.

Development of glioblastoma organoids and their applications in personalized therapy.

Glioblastomas (GBMs) are the brain tumors with the highest malignancy and poorest prognoses. GBM is characterized by high heterogeneity and resistance to drug treatment. Organoids are 3-dimensional cultures that are constructed in vitro and comprise cell types highly similar to those in organs or tissues in vivo, thus simulating specific structures and physiological functions of organs. Organoids have been technically developed into an advanced ex vivo disease model used in basic and preclinical research on tumors. Brain organoids, which simulate the brain microenvironment while preserving tumor heterogeneity, have been used to predict patients' therapeutic responses to antitumor drugs, thus enabling a breakthrough in glioma research. GBM organoids provide an effective supplementary model that reflects human tumors' biological characteristics and functions in vitro more directly and accurately than traditional experimental models. Therefore, GBM organoids are widely applicable in disease mechanism research, drug development and screening, and glioma precision treatments. This review focuses on the development of various GBM organoid models and their applications in identifying new individualized therapies against drug-resistant GBM.

Differential expression of the Hsf family in cassava under biotic and abiotic stresses.

Heat shock transcription factors (Hsfs) are important regulators of biotic and abiotic stress responses in plants. Currently, the Hsf gene family is not well understood in cassava, an important tropical crop. In the present study, 32 MeHsf genes were identified from the cassava genome database, which were divided into three types based on functional domain and motif distribution analyses. Analysis of the differential expression of the genes belonging to the Hsf family in cassava was carried out based on published cassava transcriptome data from tissues/organs (leaf blade, leaf midvein, lateral buds, organized embryogenic structures, friable embryogenic callus, fibrous roots, storage roots, stem, petiole, shoot apical meristem, and root apical meristem) under abiotic stress (cold, drought) or biotic stress (mealybugs. cassava brown streak disease, cassava bacterial blight). The results show the expression diversity of cassava Hsfs genes in various tissues/organs. The transcript levels of MeHsfB3a, MeHsfA6a, MeHsfA2a, and MeHsfA9b were upregulated by abiotic and biotic stresses, such as cold, drought, cassava bacterial blight, cassava brown streak disease, and mealybugs, indicating their potential roles in mediating the response of cassava plants to environment stresses. Further interaction network and co-expression analyses suggests that Hsf genes may interact with Hsp70 family members to resist environmental stresses in cassava. These results provide valuable information for future studies of the functional characterization of the MeHsf gene family.