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1. Tractography Study of the Human Brain: Sex Specific Templates and Sex Variations

   https://doi.org/10.1089/neu.2023.29130.abstracts  

   Ramazanpour, Mohammadreza; Jafari, Bahram; Bagherian, Amirhossein; Hajiaghamemar, Marzieh (August 2023, Journal of Neurotrauma)

   The human brain is sexually dimorphic and these sex differences have shown to affect brain response to trauma. We investigated the sex differences in the tract structures by studying diffusion weighted (DW) images of 594 females and 506 males from the Human-Connectome-Project dataset. All the female and male DW images were reconstructed in the ICBM152 space using Q-Space diffeomorphic reconstruction technique and their mapped orientation distribution function images were averaged to generate the female- and male-DW-templates. The tract streamlines were generated through tractography for female and male templates and normalized to the total brain volume . The distributions of normalized tract lengths were significantly different between female- and male-templates and the female-template showed to have more longer normalized tracts compared to the male template. For the regional analysis, the templates were parcellated into sixteen regions of interests (ROI) including brain-stem, five subregions of corpus-callosum, and right and left hippocampus, thalamus, cerebellum white-matter (WM), cerebral WM, and cerebellum cortex using a FreeSurfer-based segmentation atlas. For all the ROIs, the average fractional anisotropy (0.5-5.7%) and normalized tract lengths (1.1-2.7%) were larger in female template while the average mean diffusion was larger (1.3-5.6%) in male-template. Quantifying brain connectivity by counting number of tracts passing through pairs of ROIs, showed more pairs with a higher connectivity in female-template, and one of the highest percentages of sex differences in right/left cerebellum WM/cortex connections. Our results reinforce the need to continue investigating the sex variations in axonal structure and their effects to brain trauma. 

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2. Investigating Sex-Related Multi-Scale Brain Structural Differences and Developing Templates for Studying Traumatic Brain Injury

   https://doi.org/10.1089/neu.2024.41112.abstracts  

   Jafari, Bahram; Memar, Marzieh (August 2024, Journal of Neurotrauma)

   Sex differences in brain structure significantly influence traumatic brain injury (TBI) onset and progression, yet this area is understudied. Herein, we developed sex-specific brain anatomical (macroscale) and axonal tract (mesoscale) templates and explored the sex variations at subject level using a set of T1-MRI (609 males, 721 females) and DTI images (506 males, 594 females). The FreeSurfer, ANTs, and DSI-Studio packages were used. We investigated overall/regional volumes, DTI metrics (including fractional anisotropy (FA), mean diffusivity, and radial diffusivity), and connectivity matrix across 23 brain regions. The brain connectome was derived by multiplying the fiber tract counts and the FA values within the connecting tracts, quantifying the connection strength within each pair of regions. Our subject-wise analysis revealed significant sex based differences (Mann-Whitney p-values < 0.05) across most studied regions for all parameters. The largest sex differences in brain connections were observed in five regions: corpus callosum and right/left cortex and cerebral white matter, all stronger in females. Brain regions were typically larger in males, yet females had higher fractional volumes in the majority of regions except for CSF and ventricles, known for their cushioning effect during head impacts. Additionally, the sex-specific templates better represented their targeted sex compared to opposite or mixed-sex populations as evaluated by root-mean-square-errors when comparing the DTI metrics and connectivity from the DTI templates against the median of subjects and deformation field in registering the subjects to the T1-MRI templates. Our findings highlight the necessity of sex-specific templates in accurate brain modeling and TBI research. 

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3. Exploring the Potential Role of Sex-Based Brain Structural Variations in Susceptibility to Traumatic Brain Injury from a Biomechanics Perspective

   Jafari, Bahram; Memar, Marzieh (June 2024, SB3C2024 Summer Biomechanics, Bioengineering and Biotransport Conference)

   In this study, we aim to investigate the anatomical features and volumetric measurements of brain (macroscale), along with diffusion tensor imaging (DTI) metrics and the connections between brain regions (mesoscale), to explore sex-specific variations in the brain structure from biomechanics perspective. Such information is crucial for future studies involving FEMs in the field of brain biomechanics particularly when examining the impact of sex-specific differences on the onset and outcomes of TBI. 

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4. Sex-biased Transcriptome in in vitro Produced Bovine Early Embryos

   https://doi.org/10.1101/2025.03.04.641446  

   Shi, Meihong; Li, Guangsheng; Araujo, Hannah Marie; Lee, Angie S; Zhang, Jingzhi; Lee, Yoke Lee; Cheong, Soon Hon; Duan, Jingyue Ellie (March 2025, bioRxiv)

   Abstract BackgroundMorphologic sex differences between males and females typically emerge after the primordial germ cell migration and gonad formation, although sex is determined at fertilization based on chromosome composition. A key debated sexual difference is the embryonic developmental rate, within vitroproduced male embryos often developing faster. However, the molecular mechanisms driving early embryonic sex differences remain unclear. ResultsTo investigate the transcriptional sex difference during early development,in vitroproduced bovine blastocysts were collected and sexed by PCR. A significant male-biased development was observed in expanded blastocysts. Ultra-low input RNA-seq analysis identified 837 DEGs, with 231 upregulated and 606 downregulated in males. Functional enrichment analysis revealed male-biased DEGs were associated with metabolic regulation, whereas female-biased DEGs were related to female gonad development, sex differentiation, inflammatory pathways, and TGF-beta signaling. Comparing X chromosome and autosome expression ratio, we found that female-biased DEGs contributed to the higher X-linked gene dosage, a phenomenon not observed in male embryos. Moreover, we identified the sex-biased transcription factors and RNA-bind proteins, including pluripotent factors such asSOX21andPRDM14, and splicing factorsFMR1andHNRNPH2. Additionally, we revealed 1,555 significantly sex-biased differential alternative splicing (AS), predominantly skipped exons, mapped to 906 genes, with 59 overlapping with DEGs enriched in metabolic and autophagy pathways. By incorporating novel isoforms from long reads sequencing, we identified 1,151 sex-biased differentially expressed isoforms (DEIs) associated with 1,017 genes. Functional analysis showed that female-biased DEIs were involved in the negative regulation of transcriptional activity, while male-biased DEIs were related to energy metabolism. Furthermore, we identified sex-biased differential exon usage inDENND1B, DIS3L2, DOCK11, IL1RAPL2,andZRSR2Y,indicating their sex-specific regulation in early embryo development. ConclusionThis study provided a comprehensive analysis of transcriptome differences between male and female bovine blastocysts, integrating sex-biased gene expression, alternative splicing, and isoform dynamics. Our findings indicate that enriched metabolism processes in male embryos may contribute to the faster developmental pace, providing insights into sex-specific regulatory mechanisms during early embryogenesis. Plain English summaryMale and female early embryos develop at different speeds, with male embryos often developing faster than female embryos. However, the reasons behind these early differences remain unclear. In this study, we examined gene activity in bovine embryos to uncover the biological factors regulating these early sex differences. We collected in vitro-produced bovine blastocysts, examined their sex, and confirmed that male embryos develop faster. By analyzing global gene activity, including alternative splicing, which allows one gene to code for multiple RNA isoforms and proteins, we found distinct gene expression profiles between male and female embryos. Male embryos showed higher activity in genes related to metabolism and cellular functions, while female embryos had increased activity in genes associated with female-specific gonad development and gene expression regulation. We also examined differences in how genes on the X chromosome were expressed. Female embryos had higher X-linked gene expression, which may contribute to sex-specific developmental regulation. Additionally, we identified sex-specific transcription factors and RNA-binding proteins that regulate early embryo development, some of which are known to control pluripotency and gene splicing. Overall, our study provides new insights into how gene activity shapes early sex differences, suggesting that enhanced metabolism in male embryos may be a key driver of their faster developmental rate. HighlightsMale embryos develop faster due to increased gene expression in metabolism pathwaysFemale embryos exhibit higher X-linked gene expression, suggesting X-dosage compensation plays a role in early developmentSex-biased alternative splicing events contribute to embryonic metabolism, autophagy, and transcriptional regulation in embryosSex-biased isoform diversity contributes to distinct developmental regulation in male and female embryosKey pluripotency factors (SOX21, PRDM14) and splicing regulators (FMR1, HNRNPH2) drive sex-specific gene expression 

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5. Statistical Atlases and Automatic Labeling Strategies to Accelerate the Analysis of Social Insect Brain Evolution

   https://doi.org/10.3389/fevo.2021.745707  

   Arganda, Sara; Arganda-Carreras, Ignacio; Gordon, Darcy G.; Hoadley, Andrew P.; Pérez-Escudero, Alfonso; Giurfa, Martin; Traniello, James F. (February 2022, Frontiers in Ecology and Evolution)

   Current methods used to quantify brain size and compartmental scaling relationships in studies of social insect brain evolution involve manual annotations of images from histological samples, confocal microscopy or other sources. This process is susceptible to human bias and error and requires time-consuming effort by expert annotators. Standardized brain atlases, constructed through 3D registration and automatic segmentation, surmount these issues while increasing throughput to robustly sample diverse morphological and behavioral phenotypes. Here we design and evaluate three strategies to construct statistical brain atlases, or templates, using ants as a model taxon. The first technique creates a template by registering multiple brains of the same species. Brain regions are manually annotated on the template, and the labels are transformed back to each individual brain to obtain an automatic annotation, or to any other brain aligned with the template. The second strategy also creates a template from multiple brain images but obtains labels as a consensus from multiple manual annotations of individual brains comprising the template. The third technique is based on a template comprising brains from multiple species and the consensus of their labels. We used volume similarity as a metric to evaluate the automatic segmentation produced by each method against the inter- and intra-individual variability of human expert annotators. We found that automatic and manual methods are equivalent in volume accuracy, making the template technique an extraordinary tool to accelerate data collection and reduce human bias in the study of the evolutionary neurobiology of ants and other insects. 

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