Nature Search

Glioblastoma shift from bulk to infiltrative growth is guided by plexin-B2-mediated microglia alignment in invasive niches

Kang et al. define distinct spatial niches within glioblastoma (GBM) tumors according to their infiltrative nature and report that glioma cells induce microglia and macrophage alignments through plexin-B2 signaling, sustaining the invasive behavior of GBM.

Sangjo Kang
Mary E. Ughetta
Hongyan Zou
Research29 May 2025
Nature Cancer

Volume: 6, P: 1505-1523
Author Correction: Long-term behavioral and cell-type-specific molecular effects of early life stress are mediated by H3K79me2 dynamics in medium spiny neurons

Hope Kronman
Angélica Torres-Berrío
Eric J. Nestler
Amendments and Corrections08 Apr 2021
Nature Neuroscience

Volume: 24, P: 753-754
Bidirectional histone monoaminylation dynamics regulate neural rhythmicity

TG2 functions as an eraser and exchanger of H3 monoaminylations, including histaminylation of Gln5 of histone H3.

Qingfei Zheng
Benjamin H. Weekley
Ian Maze
ResearchOpen Access08 Jan 2025
Nature

Volume: 637, P: 974-982
Circulating myeloid-derived MMP8 in stress susceptibility and depression

Serum MMP8 is increased in stress-susceptible mice following chronic stress and leads to brain structure and behavioural changes in mice.

Flurin Cathomas
Hsiao-Yun Lin
Scott J. Russo
ResearchOpen Access07 Feb 2024
Nature

Volume: 626, P: 1108-1115
Histone serotonylation in dorsal raphe nucleus contributes to stress- and antidepressant-mediated gene expression and behavior

Serotonin is implicated in mood-related disorders, yet direct evidence linking it to disease precipitation or treatment remains limited. Here, authors show that histone serotonylation contributes to stress- and antidepressant-mediated phenotypes, which may be of clinical relevance.

Amni Al-Kachak
Giuseppina Di Salvo
Ian Maze
ResearchOpen Access13 Jun 2024
Nature Communications

Volume: 15, P: 1-17
Chromatin profiling in human neurons reveals aberrant roles for histone acetylation and BET family proteins in schizophrenia

Schizophrenia (SZ) is a severe psychiatric disorder; unfortunately, only ~1/3 of patients respond favorably to treatment. Here, the authors reveal hyperacetylation of histone H2A.Z in SZ neurons and postmortem SZ human brain tissues. They further show BRD4 is a reader of hyperacetylated H2A.Z and treatment with bromodomain inhibitor JQ1 largely rescues abnormal gene expression associated with SZ.

Lorna A. Farrelly
Shuangping Zheng
Ian Maze
ResearchOpen Access22 Apr 2022
Nature Communications

Volume: 13, P: 1-10
Author Correction: Oxycodone withdrawal induces HDAC1/HDAC2-dependent transcriptional maladaptations in the reward pathway in a mouse model of peripheral nerve injury

Kerri D. Pryce
Randal A. Serafini
Venetia Zachariou
Amendments and Corrections22 Jan 2024
Nature Neuroscience

Volume: 27, P: 384
Oxycodone withdrawal induces HDAC1/HDAC2-dependent transcriptional maladaptations in the reward pathway in a mouse model of peripheral nerve injury

Oxycodone withdrawal triggered distinct transcriptomic changes in the ventral tegmental area, nucleus accumbens and medial prefrontal cortex in mice with and without chronic pain, with histone deacetylase 1 (HDAC1) as a common upstream regulator. A novel HDAC1/HDAC2 inhibitor reduced behavioral manifestations of oxycodone withdrawal.

Kerri D. Pryce
Randal A. Serafini
Venetia Zachariou
Research08 Jun 2023
Nature Neuroscience

Volume: 26, P: 1229-1244
Circadian clock regulator Bmal1 gates axon regeneration via Tet3 epigenetics in mouse sensory neurons

Injured peripheral neurons activate pro-growth gene programs, yet the mechanisms remain unclear. Here, the authors show that disruption of circadian clock factor Bmal1 accelerates axon regeneration through augmented epigenetic responses after injury.

Dalia Halawani
Yiqun Wang
Hongyan Zou
ResearchOpen Access24 Aug 2023
Nature Communications

Volume: 14, P: 1-22
Early life stress alters transcriptomic patterning across reward circuitry in male and female mice

Early life stress alters behavioural response to adult stress in female mice. Here authors transcriptionally profile three brain regions involved in reward (ventral tegmental area, nucleus accumbens, and prefrontal cortex) in both male and female adult mice after early life and/or adult stress

Catherine Jensen Peña
Milo Smith
Eric J. Nestler
ResearchOpen Access08 Nov 2019
Nature Communications

Volume: 10, P: 1-13
Stress resilience is promoted by a Zfp189-driven transcriptional network in prefrontal cortex

Researchers identify a transcriptional network engaged in stress-resilient mice that is regulated by a previously unstudied transcription factor, Zfp189, and elucidate molecular mechanisms controlling this network and resilience behavior.

Zachary S. Lorsch
Peter J. Hamilton
Eric J. Nestler
Research19 Aug 2019
Nature Neuroscience

Volume: 22, P: 1413-1423
Rescue of deficits by Brwd1 copy number restoration in the Ts65Dn mouse model of Down syndrome

The molecular mechanisms underlying deficits in Down syndrome remain unclear. Here, the authors show that copy number restoration of a chromatin remodeler in trisomic mice is sufficient to rescue epigenomic, physiological and cognitive deficits.

Sasha L. Fulton
Wendy Wenderski
Ian Maze
ResearchOpen Access26 Oct 2022
Nature Communications

Volume: 13, P: 1-17
Long-term behavioral and cell-type-specific molecular effects of early life stress are mediated by H3K79me2 dynamics in medium spiny neurons

Early life stress (ELS) promotes susceptibility to the effects of chronic stress in adulthood. Kronman et al. show that ELS alters H3K79me2 in D2 medium spiny neurons in the nucleus accumbens and that this underlies the susceptibility to the effects of subsequent stress.

Hope Kronman
Angélica Torres-Berrío
Eric J. Nestler
Research15 Mar 2021
Nature Neuroscience

Volume: 24, P: 667-676
Plexin-B2 orchestrates collective stem cell dynamics via actomyosin contractility, cytoskeletal tension and adhesion

Biomechanical mechanisms orchestrating stem cell dynamics in development remain unclear. Here the authors show that guidance receptor Plexin-B2 organizes actomyosin contractility, cytoskeletal tension and adhesion during multicellular development of human embryonic stem cells and neuroprogenitor cells.

Chrystian Junqueira Alves
Rafael Dariolli
Roland H. Friedel
ResearchOpen Access14 Oct 2021
Nature Communications

Volume: 12, P: 1-23
Neocortical tau propagation is a mediator of clinical heterogeneity in Alzheimer’s disease

Anjalika Chongtham
Aarthi Ramakrishnan
Ana C. Pereira
Research16 Apr 2025
Molecular Psychiatry

Volume: 30, P: 4194-4213
Histone serotonylation is a permissive modification that enhances TFIID binding to H3K4me3

In serotonin-rich tissues, tissue transglutaminase 2 is able to attach serotonin to a glutamine residue in histone H3; this modification mediates permissive gene expression in these tissues.

Lorna A. Farrelly
Robert E. Thompson
Ian Maze
Research13 Mar 2019
Nature

Volume: 567, P: 535-539
Glycan topology determines human adaptation of avian H5N1 virus hemagglutinin

Aarthi Chandrasekaran
Aravind Srinivasan
Ram Sasisekharan
Research06 Jan 2008
Nature Biotechnology

Volume: 26, P: 107-113
Hypoxia drives shared and distinct transcriptomic changes in two invasive glioma stem cell lines

Valerie J. Marallano
Mary E. Ughetta
Roland H. Friedel
ResearchOpen Access27 Mar 2024
Scientific Reports

Volume: 14, P: 1-12
Blood miR-144-3p: a novel diagnostic and therapeutic tool for depression

Yentl Y. van der Zee
Lars M. T. Eijssen
Orna Issler
Research28 Jul 2022
Molecular Psychiatry

Volume: 27, P: 4536-4549
Whole blood transcriptional signatures associated with rapid antidepressant response to ketamine in patients with treatment resistant depression

Flurin Cathomas
Laura Bevilacqua
James W. Murrough
ResearchOpen Access10 Jan 2022
Translational Psychiatry

Volume: 12, P: 1-9

Search

Glioblastoma shift from bulk to infiltrative growth is guided by plexin-B2-mediated microglia alignment in invasive niches

Author Correction: Long-term behavioral and cell-type-specific molecular effects of early life stress are mediated by H3K79me2 dynamics in medium spiny neurons

Bidirectional histone monoaminylation dynamics regulate neural rhythmicity

Circulating myeloid-derived MMP8 in stress susceptibility and depression

Histone serotonylation in dorsal raphe nucleus contributes to stress- and antidepressant-mediated gene expression and behavior

Chromatin profiling in human neurons reveals aberrant roles for histone acetylation and BET family proteins in schizophrenia

Author Correction: Oxycodone withdrawal induces HDAC1/HDAC2-dependent transcriptional maladaptations in the reward pathway in a mouse model of peripheral nerve injury

Oxycodone withdrawal induces HDAC1/HDAC2-dependent transcriptional maladaptations in the reward pathway in a mouse model of peripheral nerve injury

Circadian clock regulator Bmal1 gates axon regeneration via Tet3 epigenetics in mouse sensory neurons

Early life stress alters transcriptomic patterning across reward circuitry in male and female mice

Stress resilience is promoted by a Zfp189-driven transcriptional network in prefrontal cortex

Rescue of deficits by Brwd1 copy number restoration in the Ts65Dn mouse model of Down syndrome

Long-term behavioral and cell-type-specific molecular effects of early life stress are mediated by H3K79me2 dynamics in medium spiny neurons

Plexin-B2 orchestrates collective stem cell dynamics via actomyosin contractility, cytoskeletal tension and adhesion

Neocortical tau propagation is a mediator of clinical heterogeneity in Alzheimer’s disease

Histone serotonylation is a permissive modification that enhances TFIID binding to H3K4me3

Glycan topology determines human adaptation of avian H5N1 virus hemagglutinin

Hypoxia drives shared and distinct transcriptomic changes in two invasive glioma stem cell lines

Blood miR-144-3p: a novel diagnostic and therapeutic tool for depression

Whole blood transcriptional signatures associated with rapid antidepressant response to ketamine in patients with treatment resistant depression

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