bims-nimamd Biomed News
on Neuroimmunity and neuroinflammation in ageing and metabolic disease
Issue of 2026–02–15
29 papers selected by
Fawaz Alzaïd, Sorbonne Université
  1. Distinct spatial organization governs oral mucosal immunity.
  2. Virtual assistant enhances health outcomes in older adults with type 2 diabetes.
  3. PD-1 blockade reprograms antiviral immunity and reduces the HIV reservoir.
  4. Endogenous retroviruses help activate the human zygotic genome.
  5. Gut macrophages and Parkinson's disease.
  6. The bottleneck of fat burning.
  7. Implementing a nationwide healthy longevity program for older adults.
  8. Exercise rewires the brain - boosting the body's endurance.
  9. The invisible scientist.
  10. Integrated histopathology of the human pancreas throughout stages of type 1 diabetes progression.
  11. Tissue-resident macrophage survival depends on mitochondrial function regulated by SerpinB2 in chronic inflammation.
  12. The 'astounding' rise of semaglutide - and what's next for weight-loss drugs.
  13. Coffee linked to slower brain ageing in study of 130,000 people.
  14. Partitioned polygenic scores show mechanistic heterogeneity in type 2 diabetes and hypertension comorbidity.
  15. Microglia makeover: On-demand control panel revamp.
  16. Capillary blood sampling for detecting biomarkers of Alzheimer's disease.
  17. Lack of MDA5 delays hematopoietic aging by modulating inflammaging and proteostasis in mice.
  18. Intrinsic and niche-dependent metabolic regulation of haematopoietic stem cells and implications for leukaemogenesis.
  19. O-GlcNAcylation shapes macrophage tissue residency and alternative activation.
  20. Deep-coverage single-cell metabolomics enabled by ion mobility-resolved mass cytometry.
  21. Robust partitioning of cell contents by physical instabilities and biological clocks.
  22. Dozens of researchers will move to France from US following high-profile bid to lure talent.
  23. TCRγ constant usage tunes human γδ T cell antigen sensitivity, thymic programming, and peripheral function.
  24. Clearing trapped cholesterol could relieve lymphoedema.
  25. TCRAFT: A Rosetta Stone for T cell receptors.
  26. MYC modulates TOP2A diffusion to promote substrate detection and activity.
  27. These hungry immune cells tidy sleeping flies' brains.
  28. Identifying 3D signal overlaps in spatial transcriptomics data with ovrlpy.
  29. Structural basis of TACO1-mediated efficient mitochondrial translation.
  1. Nat Immunol. 2026 Feb 11.
    Distinct spatial organization governs oral mucosal immunity.
      
    DOI:  https://doi.org/10.1038/s41590-025-02410-5
  2. Nat Aging. 2026 Feb 12.
    Virtual assistant enhances health outcomes in older adults with type 2 diabetes.
    Yahyah Aman.
      
    DOI:  https://doi.org/10.1038/s43587-026-01083-5
  3. Nat Med. 2026 Feb 12.
    PD-1 blockade reprograms antiviral immunity and reduces the HIV reservoir.
      
    DOI:  https://doi.org/10.1038/s41591-025-04152-1
  4. Nat Genet. 2026 Feb;58(2): 240
    Endogenous retroviruses help activate the human zygotic genome.
    Tiago Faial.
      
    DOI:  https://doi.org/10.1038/s41588-026-02527-9
  5. Nat Rev Immunol. 2026 Feb 11.
    Gut macrophages and Parkinson's disease.
    Yvonne Bordon.
      
    DOI:  https://doi.org/10.1038/s41577-026-01281-7
  6. Science. 2026 Feb 12. 391(6786): 659-660
    The bottleneck of fat burning.
    Angela M Ramos-Lobo, Pierre Maechler.
      A mitochondrial transport protein promotes carnitine synthesis in mice when fat consumption is needed.
    DOI:  https://doi.org/10.1126/science.aef2173
  7. Nat Aging. 2026 Feb 11.
    Implementing a nationwide healthy longevity program for older adults.
    Bruno Vellas.
      
    DOI:  https://doi.org/10.1038/s43587-026-01080-8
  8. Nature. 2026 Feb 12.
    Exercise rewires the brain - boosting the body's endurance.
    Mariana Lenharo.
      
    Keywords:  Brain; Neuroscience; Physiology
    DOI:  https://doi.org/10.1038/d41586-026-00414-1
  9. Science. 2026 Feb 12. 391(6786): 738
    The invisible scientist.
    Anne Trolard.
      
    DOI:  https://doi.org/10.1126/science.aeg2379
  10. Nat Commun. 2026 Feb 11.
    Integrated histopathology of the human pancreas throughout stages of type 1 diabetes progression.
    Verena van der Heide, Sara McArdle, Michael S Nelson, Karen Cerosaletti, Sacha Gnjatic, Zbigniew Mikulski, Amanda L Posgai, Irina Kusmartseva, Mark A Atkinson, Dirk Homann.
      Type 1 diabetes (T1D) is a progressive autoimmune condition that culminates in loss of insulin-producing beta cells. Pancreatic histopathology provides essential insights into disease initiation/progression yet an integrated perspective onto in situ pathogenic processes is lacking. Here, we combined multiplexed immunostaining, high-magnification whole-slide imaging, digital pathology, and semi-automated image analyses to interrogate pancreatic tail and head sections across T1D stages, including at-risk and at-onset cases. Deconvolution of architectural features, endocrine cell composition, immune cell burden, and spatial relations of ~25,000 islets effectively contextualizes previously established and additional pancreatic hallmarks in health and T1D. Our results reveal a spatially homogenous and islet size-contingent architectural organization of the endocrine pancreas, a notable coordination of organ-wide pathogenic processes, and multiple histopathological correlates that foreshadow distinctive T1D histopathology already at the preclinical stage. Altogether, we propose a revised natural history of T1D with implications for further histopathological investigations and considerations of pathogenetic modalities.
    DOI:  https://doi.org/10.1038/s41467-026-68610-1
  11. Nat Commun. 2026 Feb 12. 17(1): 1493
    Tissue-resident macrophage survival depends on mitochondrial function regulated by SerpinB2 in chronic inflammation.
    Sathish Babu Vasamsetti, Samreen Sadaf, Mohammad A Uddin, Jixing Shen, Ebin Johny, Awishi Mondal, Jonathan Florentin, Liqun Lei, Aleef Mannan, Krithika Sudhakar Rao, John Sembrat, Mauricio Rojas, Ian Sipula, Jake Kastroll, Michael J Jurczak, Sruti Shiva, Robert M O'Doherty, Vijay Yechoor, Partha Dutta.
      How cellular metabolism facilitates tissue-resident macrophage maintenance remains elusive. Here we show that visceral adipose tissue (VAT)-resident macrophages, unlike monocyte-derived macrophages, are enriched with mitochondrial-specific antioxidant enzymes restraining inflammation and promoting VAT homeostasis and insulin sensitivity. Additionally, VAT resident macrophages express high levels of plasminogen activator inhibitor type 2, encoded by SerpinB2, which is involved in the blood coagulation cascade. SerpinB2 promotes adipose resident macrophage survival by regulating mitochondrial oxidative phosphorylation and preventing the release of pro-apoptotic cytochrome c from the mitochondria into the cytoplasm via antioxidant glutathione production. Chronic inflammation, such as obesity, diminishes SerpinB2 expression in VAT macrophages in patients and mice, leading to the decline of this macrophage subset. Mechanistically, interferon-γ elevation in diabetes induces Ikaros, a transcriptional suppressor, which binds to the SerpinB2 promoter and decreases SerpinB2 expression. Congruently, selective depletion of the IFN-γ receptor in myeloid cells or supplementation of macrophage-specific SerpinB2 deficient mice with N-acetylcysteine, a glutathione precursor, restores VAT resident macrophage survival, decreases adipocyte size, and improves glucose tolerance and insulin sensitivity. Our data thus reveal an unexpected function of SerpinB2 in the regulation of mitochondrial function and survival of tissue-resident macrophages.
    DOI:  https://doi.org/10.1038/s41467-026-69196-4
  12. Nature. 2026 Feb 12.
    The 'astounding' rise of semaglutide - and what's next for weight-loss drugs.
    Bianca Nogrady.
      
    Keywords:  Diabetes; Metabolism; Obesity; Public health; Society; Technology
    DOI:  https://doi.org/10.1038/d41586-026-00228-1
  13. Nature. 2026 Feb 09.
    Coffee linked to slower brain ageing in study of 130,000 people.
    Amanda Heidt.
      
    Keywords:  Ageing; Alzheimer's disease; Nutrition; Public health
    DOI:  https://doi.org/10.1038/d41586-026-00409-y
  14. Nat Commun. 2026 Feb 09. 17(1): 1446
    Partitioned polygenic scores show mechanistic heterogeneity in type 2 diabetes and hypertension comorbidity.
    Vincent Pascat, Liudmila Zudina, Lucas Maurin, Anna Ulrich, Jared G Maina, Ayse Demirkan, Zhanna Balkhiyarova, Igor Pupko, Yevheniya Sharhorodska, François Pattou, Bart Staels, Marika Kaakinen, Amna Khamis, Amélie Bonnefond, Patricia Munroe, Philippe Froguel, Inga Prokopenko.
      Type 2 diabetes and hypertension are common health conditions that often occur together, suggesting shared biological mechanisms. To explore this relationship, we analyse large-scale multiomic data to uncover genetic factors underlying type 2 diabetes and blood pressure comorbidity. We curate 1304 independent single-nucleotide variants associated with type 2 diabetes and blood pressure, grouping them into five clusters related to metabolic syndrome, inverse type 2 diabetes/blood pressure risk, impaired pancreatic beta-cell function, higher adiposity, and vascular dysfunction. Colocalization with tissue-specific gene expression highlights significant enrichment in pathways related to thyroid function and fetal development. Partitioned polygenic scores derived from these clusters improve risk prediction for type 2 diabetes/hypertension comorbidity, identifying individuals with more than twice the usual susceptibility. These results reveal a mechanistically heterogeneous genetic architecture shared between type 2 diabetes and blood pressure, enhancing comorbidity risk prediction. Partitioned polygenic risk scores offer a promising approach for early risk stratification, personalised prevention, and improved management of these interconnected conditions.
    DOI:  https://doi.org/10.1038/s41467-025-67449-2
  15. Immunity. 2026 Feb 10. pii: S1074-7613(26)00028-2. [Epub ahead of print]59(2): 229-231
    Microglia makeover: On-demand control panel revamp.
    Takahiro Masuda.
      Microglia display remarkable plasticity, with their cellular states evolving in response to developmental stage, regional context, and environmental or pathological stimuli. In this issue of Immunity, Hamagami et al. demonstrate that adaptive reconfiguration of regulatory networks, particularly the dynamics of enhancers, underlies these state transitions. Conserved enhancers link developmental and Alzheimer's-related microglial states, suggesting shared epigenetic frameworks that influence neurodegenerative susceptibility.
    DOI:  https://doi.org/10.1016/j.immuni.2026.01.007
  16. Nat Med. 2026 Feb 11.
    Capillary blood sampling for detecting biomarkers of Alzheimer's disease.
      
    DOI:  https://doi.org/10.1038/s41591-026-04216-w
  17. Nat Commun. 2026 Feb 12. 17(1): 1645
    Lack of MDA5 delays hematopoietic aging by modulating inflammaging and proteostasis in mice.
    Veronica Bergo, Pavlos Bousounis, Giang To Vu, Mélodie Douté, Aikaterini Polyzou, Maria-Eleni Lalioti, Bogdan B Grigorash, Lyudmila Tsurkan, Nicholas Morchel, Ward Deboutte, Frédéric Brau, Thomas Manke, Sagar, Hind Medyouf, Dmitry V Bulavin, Nina Cabezas-Wallscheid, Marta Derecka, Eirini Trompouki.
      "Inflammaging", the chronic increase in inflammatory signaling with age, remains poorly understood in hematopoietic aging. Here, we identify the innate immune RNA sensor melanoma differentiation-associated protein 5 (MDA5) as an important factor of hematopoietic stem cell (HSC) aging. Aged Mda5-/- mice exhibit reduced HSC accumulation and myeloid bias. Importantly, aged Mda5-/- HSCs retain greater quiescence and superior repopulation capacity in noncompetitive transplants compared to wild-type counterparts. Multiomic analyses- including chromatin accessibility, transcriptomics, and metabolomics-reveal decreased inflammatory signaling, a youthful metabolic profile, and improved proteostasis in Mda5-/- HSCs, through regulation of HSF1 and phospho-EIF2A, key proteostasis regulators. Activation of HSF1 in aged wild-type HSCs partially restores youthful features, supporting a causal role for proteostasis maintenance. Collectively, our findings demonstrate that attenuating MDA5-dependent inflammation preserves HSC function during aging by maintaining metabolic fitness and proteostasis and provide insight into potential therapeutic strategies for mitigating hematopoietic aging.
    DOI:  https://doi.org/10.1038/s41467-026-69424-x
  18. Nat Cell Biol. 2026 Feb 11.
    Intrinsic and niche-dependent metabolic regulation of haematopoietic stem cells and implications for leukaemogenesis.
    Ayşegül Erdem, Claudia Morganti, Haruhito Totani, Nick van Gastel, Keisuke Ito.
      Haematopoietic stem cells (HSCs) rely on precisely coordinated metabolic programs to preserve their functionality, adapt to environmental cues, and sustain lifelong haematopoiesis. Here we analyse recent advances in understanding the metabolic landscape of HSCs, emphasizing how their intrinsic bioenergetic programs facilitate quiescence, self-renewal and differentiation. We also summarize the dynamic metabolic interactions with the bone marrow microenvironment, including stromal cells, osteoblasts, endosteal cells and adipose tissue, highlighting how they support proper HSC fate. In addition, we discuss how alterations in metabolic homeostasis in healthy and aged HSCs are linked to haematological disorders, particularly leukaemogenesis. We discuss metabolic dysregulation in leukaemic cells that maintains malignant persistence by mimicking certain intrinsic-extrinsic key HSC metabolic features, while simultaneously activating distinct metabolic pathways to support their growth and survival. Understanding the complex role of metabolism in HSC biology will be essential to advance regenerative medicine and blood cancer prevention strategies.
    DOI:  https://doi.org/10.1038/s41556-026-01872-5
  19. Nat Rev Immunol. 2026 Feb 10.
    O-GlcNAcylation shapes macrophage tissue residency and alternative activation.
    Amitava Sinha, Thomas Weichhart.
      
    DOI:  https://doi.org/10.1038/s41577-026-01278-2
  20. Nat Methods. 2026 Feb 09.
    Deep-coverage single-cell metabolomics enabled by ion mobility-resolved mass cytometry.
    Mingdu Luo, Tianzhang Kou, Yandong Yin, Shengyi Zhou, Xiaolan Zhu, Xinhao Zeng, Junhao Hu, Zheng-Jiang Zhu.
      Current single-cell metabolomics approaches are limited by insufficient sensitivity, robustness and metabolite coverage. We present an ion mobility-resolved mass cytometry technology that integrates high-throughput single-cell injection with ion mobility-mass spectrometry for multidimensional metabolomic profiling. Ion mobility-enabled selective ion accumulation and cell superposition-based amplification strategies substantially enhance sensitivity, robustness and overall analytical performance. Combined with our computational tool, MetCell, this technology allows high-throughput analysis while achieving exceptional profiling depth, detecting over 5,000 metabolic peaks and annotating approximately 800 metabolites per cell-representing a 3-fold to 10-fold improvement over existing methods. It offers attomole-level sensitivity and captures a broad dynamic range of metabolites within individual cells. Applied to 45,603 primary liver cells from aging mice, it enabled accurate cell-type and cell-subtype annotation and revealed distinct metabolic states and heterogeneity in hepatocytes during aging. This platform sets a new benchmark for high-throughput single-cell metabolomics, advancing our understanding of metabolic heterogeneity at single-cell resolution.
    DOI:  https://doi.org/10.1038/s41592-025-02970-2
  21. Nature. 2026 Feb 11.
    Robust partitioning of cell contents by physical instabilities and biological clocks.
      
    Keywords:  Cell biology; Developmental biology
    DOI:  https://doi.org/10.1038/d41586-026-00021-0
  22. Nature. 2026 Feb 10.
    Dozens of researchers will move to France from US following high-profile bid to lure talent.
    Elizabeth Gibney, Max Kozlov.
      
    Keywords:  Funding; Government; Scientific community
    DOI:  https://doi.org/10.1038/d41586-026-00405-2
  23. Sci Immunol. 2026 Feb 13. 11(116): eadr7167
    TCRγ constant usage tunes human γδ T cell antigen sensitivity, thymic programming, and peripheral function.
    Mayuri Viswanathan, Caitlin D Castro, Augusta E Broughton, Amrita Ramesh, Nicholas Asby, Alejandra Bergquist, Caroline Kaiser, Alexander Luna, Jun Huang, Marc Bissonnette, Andrew Koh, Narutoshi Hibino, Nathan Schoettler, Anne Sperling, Erin J Adams.
      Activation in T cells through their antigen receptors has been closely tied to the strength of recognition of their cognate antigens, dictated by the variable complementarity-determining region loops. We show that, in the human gamma delta (γδ) T cell receptors (TCRs), the gamma constant domains modulate activation intensity independent of variable region antigen recognition. Using single-cell RNA sequencing data, we demonstrate that Cγ usage in vivo corresponds with distinct phenotypes, with cells using Cγ1 having a more differentiated cytotoxic effector phenotype in the thymus and higher granzyme expression in peripheral tissues. TCRs with Cγ1 are also selectively expanded in colorectal tumors. Cγ2 usage is correlated with naïve phenotypes in development and with inhibition and wound healing in the periphery. We propose that the modulation of activation using Cγ1 or Cγ2 translates to differences in γδ T cell phenotype and clonal expansion throughout its life span, providing human γδ T cells another "dial" to modulate their function.
    DOI:  https://doi.org/10.1126/sciimmunol.adr7167
  24. Nature. 2026 Feb 11.
    Clearing trapped cholesterol could relieve lymphoedema.
    Babak Mehrara.
      
    Keywords:  Medical research; Metabolism; Physiology
    DOI:  https://doi.org/10.1038/d41586-026-00176-w
  25. Immunity. 2026 Feb 10. pii: S1074-7613(26)00044-0. [Epub ahead of print]59(2): 238-240
    TCRAFT: A Rosetta Stone for T cell receptors.
    Christopher A Polera, Alex M Jaeger.
      Defining the antigen specificity of T cell receptors (TCRs) remains a significant barrier to understanding adaptive immunity in various pathologies. In this issue of Immunity, Gaglione et al. report the development of TCRAFT, a novel platform that enables facile construction of vast TCR sequence libraries that can be screened against hundreds of antigens. This approach makes functional immune screening highly accessible.
    DOI:  https://doi.org/10.1016/j.immuni.2026.01.024
  26. Nat Commun. 2026 Feb 09.
    MYC modulates TOP2A diffusion to promote substrate detection and activity.
    Donald P Cameron, Kathryn Jackson, Alessia Loffreda, Carl Möller, Vladislav Kuzin, Matteo Mazzocca, Evanthia Iliopoulou, Hallgerdur Kolbeinsdottir, Andrej Paluda, Evgeniya Pavlova, Bea Jagodic, Brian Saidel Lopez Duran, Valérie Lamour, Fredrik Westerlund, Davide Mazza, Laura Baranello.
      Topoisomerases alleviate DNA supercoiling by cleaving and resealing DNA strands. Previously, we showed that the oncoprotein MYC recruits and stimulates topoisomerases to remove DNA entanglements generated by oncogenic transcription. Understanding this mechanism may suggest methods to inhibit MYC-driven topoisomerase activation, targeting tumor-specific transcription. Here, we demonstrate that the essential topoisomerase TOP2A in human cells exists in a dynamic equilibrium between sequestration in the nucleolus, substrate searching in transcription hubs, and active engagement on chromatin. This equilibrium is highly responsive to changes in DNA topology, allowing cells to regulate TOP2A levels. Using single molecule tracking, here we show that MYC accelerates TOP2A diffusion in cells. We explain this phenotype by demonstrating that MYC limits TOP2A self-interaction in vitro, while decreasing the size of TOP2A complexes in cells. By increasing TOP2A diffusion, MYC promotes substrate binding and increases TOP2A engagement on chromatin genome-wide, revealing the mechanism underlying MYC stimulation of TOP2A activity.
    DOI:  https://doi.org/10.1038/s41467-026-69232-3
  27. Nature. 2026 Feb 11.
    These hungry immune cells tidy sleeping flies' brains.
    Benjamin Thompson, Nick Petrić Howe.
      
    Keywords:  Anthropology; Brain; Immunology
    DOI:  https://doi.org/10.1038/d41586-026-00452-9
  28. Nat Biotechnol. 2026 Feb 10.
    Identifying 3D signal overlaps in spatial transcriptomics data with ovrlpy.
    Sebastian Tiesmeyer, Niklas Müller-Bötticher, Alexander Malt, Leyao Ma, Sergio Marco-Salas, Paul Kiessling, Paul Horn, Adrien Guillot, Louis B Kuemmerle, Frank Tacke, Fabian J Theis, Christoph Kuppe, Mats Nilsson, Roland Eils, Brian Long, Naveed Ishaque.
      Imaging-based spatially resolved transcriptomics can localize transcripts within tissue sections in three dimensions. However, cell segmentation, which assigns transcripts to cells, is usually performed in two dimensions and spatial doublets in the vertical dimension result in segmented cells containing transcripts originating from multiple cell types. Here we present a computational tool called ovrlpy that identifies overlapping cells, tissue folds and inaccurate cell segmentation by analyzing transcript localization in three dimensions.
    DOI:  https://doi.org/10.1038/s41587-026-03004-8
  29. Nat Commun. 2026 Feb 09.
    Structural basis of TACO1-mediated efficient mitochondrial translation.
    Shuhui Wang, Michele Brischigliaro, Yuekang Zhang, Chunxiang Wu, Wei Zheng, Antoni Barrientos, Yong Xiong.
      Translation elongation is a universally conserved step in protein synthesis, relying on elongation factors that engage the ribosomal L7/L12 stalk to mediate aminoacyl-tRNA delivery, accommodation, and ribosomal translocation. Using in organello cryo-electron microscopy, we reveal how the mitochondrial translation accelerator TACO1 promotes efficient elongation on human mitoribosomes. TACO1 binds the mitoribosomal region typically bound by elongation factor Tu (mtEF-Tu), bridging the large and small subunits via contacts with 16S rRNA, bL12m, A-site tRNA, and uS12m. While active throughout elongation, TACO1 is especially critical when translating polyproline motifs. Its absence prolongs mtEF-Tu residence in A/T states, causes persistent mitoribosomal stalling and premature subunit dissociation. Structural analyses indicate that TACO1 competes with mtEF-Tu for mitoribosome binding, stabilizes A-site tRNA, and enhances peptidyl transfer through a mechanism distinct from EF-P and eIF5A. These findings suggest that bacterial TACO1 orthologs may serve analogous roles, highlighting an evolutionarily conserved strategy for maintaining elongation efficiency during challenging translation events.
    DOI:  https://doi.org/10.1038/s41467-026-69156-y
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