DiI‐mediated analysis of presynaptic and postsynaptic structures in human postmortem brain tissue

Das, Sujan C.; Chen, Danli; Callor, W. Brandon; Christensen, Eric; Coon, Hilary; Williams, Megan E.

doi:10.1002/cne.24722

Cited by 13 publications

(21 citation statements)

References 50 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In accordance, the quantification technique only allowed for the identification of spines in the same x-y plane as the dendrite. Although the densities in the present study are comparable to those using similar methods [32], these combined factors likely underlie why the density of spines in the present study is lower than that identified using more sensitive methods in both rodents [81] and humans [82]. In the interpretation of the presented data, we acknowledge that these impacts may actually under-represent spine losses in the human OFC and the effect size may indeed be larger using techniques which facilitate greater resolution of spine detection.…”

Section: Discussioncontrasting

confidence: 49%

Severe childhood and adulthood stress associates with neocortical layer-specific reductions of mature spines in psychiatric disorders

Kaul

Smith

Stevens

et al. 2020

Preprint

View full text Add to dashboard Cite

Severe stress exposure causes the loss of dendritic spines on cortical pyramidal neurons and induces psychiatric-like symptoms in rodent models. These effects are strongest following early-life stress and are most persistent on apical dendrites. However, the long-term impacts and temporal effects of stress exposure on the human brain remain poorly understood. Using a novel postmortem cohort of psychiatric cases with severe stress experienced in childhood, adulthood, or no severe stress, and matched controls, we aimed to determine the impact of stress timing on pyramidal neuron structure in the human orbitofrontal cortex (OFC). We performed Golgi Cox staining and manually measured the morphology and density of over 22,000 dendritic spines on layer-specific pyramidal neuron apical dendrites. We also quantified glucocorticoid receptor mRNA and protein as a marker of stress dysregulation. Both childhood and adulthood stress were associated with large reductions in mature mushroom spine density (up to 56% loss) in both the superficial (II/III) and deeper layers (V) of the OFC. However, childhood stress caused more substantial reductions to both total and mature spines. No difference in glucocorticoid receptor mRNA and protein were seen between groups, although both negatively correlated with total spine density within the whole cohort. These findings indicate that severe stress, especially when experienced during childhood, persistently affects the fine morphological properties of neurons in the human OFC. This may impact on cell connectivity in this brain area, and at least partly explain the social and emotional symptoms that originate in the OFC in psychiatric disorders.

show abstract

Section: Discussioncontrasting

confidence: 49%

Severe childhood and adulthood stress associates with neocortical layer-specific reductions of mature spines in psychiatric disorders

Kaul

Smith

Stevens

et al. 2020

Preprint

View full text Add to dashboard Cite

show abstract

“…Synapse regulation is a central event during nervous system development and adult life. Disruptions in the establishment of synapses is associated with morphological, cognitive and psychiatric disorders, but the precise mechanisms underlying these disorders remain unknown [42]. Changes in synapse structure and function are related to paralysis and muscular atrophy in amyotrophic lateral sclerosis (ALS) [43,44], impairment of the neuromuscular junction function and therefore, motor decline [45] or social and cognitive behaviors related to autism [46].…”

Section: Discussionmentioning

confidence: 99%

Small heat shock proteins determine synapse number and neuronal activity during development

2020

View full text Add to dashboard Cite

Environmental changes cause stress, Reactive Oxygen Species and unfolded protein accumulation which hamper synaptic activity and trigger cell death. Heat shock proteins (HSPs) assist protein refolding to maintain proteostasis and cellular integrity. Mechanisms regulating the activity of HSPs include transcription factors and posttranslational modifications that ensure a rapid response. HSPs preserve synaptic function in the nervous system upon environmental insults or pathological factors and contribute to the coupling between environmental cues and neuron control of development. We have performed a biased screening in Drosophila melanogaster searching for synaptogenic modulators among HSPs during development. We explore the role of two small-HSPs (sHSPs), sHSP23 and sHSP26 in synaptogenesis and neuronal activity. Both sHSPs immunoprecipitate together and the equilibrium between both chaperones is required for neuronal development and activity. The molecular mechanism controlling HSP23 and HSP26 accumulation in neurons relies on a novel gene (CG1561), which we name Pinkman (pkm). We propose that sHSPs and Pkm are targets to modulate the impact of stress in neurons and to prevent synapse loss.

show abstract

“…In human neuronal disorders, the vast majority of research focuses on mature dendritic spines found in postmortem patient brain samples from adolescents and adults (Bao & Swaab, 2018; Hutsler & Zhang, 2010; Tang et al., 2014). In spite of recent techniques to minimize fixation artifacts (Das et al., 2019), postmortem brain tissue is limited to a static snapshot of synapse development. Furthermore, while rodent models capture synapse dynamics (Marrs, Green, & Dailey, 2001), most research focuses on peri‐ and postnatal periods of synaptic development.…”

Section: Introductionmentioning

confidence: 99%

Cytoskeletal regulation of synaptogenesis in a model of human fetal brain development

Wilson

Rudisill

Kirk

et al. 2020

J of Neuroscience Research

View full text Add to dashboard Cite

Synapses are specialized neural cell adhesions that underlie neurotransmission (Lynch, Rex, & Gall, 2007; Vicente-Manzanares, Hodges, & Horwitz, 2009). Synapse development is altered in the neurodevelopmental disorders of epilepsy, intellectual disability, and autism spectrum disorders (Forrest, Parnell, & Penzes, 2018). The onset of excitatory synapse formation occurs during mid-fetal gestation (Tierney & Nelson, 2009; Yuste & Bonhoeffer, 2004). Intriguingly, the expression profile of genes associated with neurodevelopmental disorders peaks in prenatal brain development (Birnbaum, Jaffe, Hyde, Kleinman, & Weinberger, 2014). However, due to our inability to image synaptogenesis in utero, prenatal brain development remains understudied. Instead, most research focuses on postnatal refinement of synaptic circuits. In order to research the molecular mechanisms of fetal synaptogenesis, we develop human cortical spheroids (HCSs). HCSs offer an unprecedented opportunity to observe the initial formation of excitatory synapses (Wilson & Newell-Litwa, 2018).

show abstract

DiI‐mediated analysis of presynaptic and postsynaptic structures in human postmortem brain tissue

Cited by 13 publications

References 50 publications

Severe childhood and adulthood stress associates with neocortical layer-specific reductions of mature spines in psychiatric disorders

Severe childhood and adulthood stress associates with neocortical layer-specific reductions of mature spines in psychiatric disorders

Small heat shock proteins determine synapse number and neuronal activity during development

Cytoskeletal regulation of synaptogenesis in a model of human fetal brain development

Contact Info

Product

Resources

About