Magnetic Resonance Imaging of Hippocampal Subfields in Posttraumatic Stress Disorder

Wang, Zhen; Neylan, Thomas C.; Mueller, Susanne; Lenoci, Maryann; Truran, Diana; Marmar, Charles R.; Weiner, Michael W.; Schuff, Norbert

doi:10.1001/archgenpsychiatry.2009.205

Cited by 265 publications

(229 citation statements)

References 63 publications

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“…8 We echo the author's sentiments that it's not evident from our current study that administration of IGF-1 will improve insomnia or attenuate comorbid symptoms. However, since there was a positive association between sleep quality improvements and IGF-1 increases, which is also confi rmed by a recent Cochrane meta-analysis, 9 it may be a treatment intervention worth exploring.…”

Section: 7supporting

confidence: 51%

Effect of Acute Sleep Disturbance and Recovery on Insulin-Like Growth Factor-1 (IGF-1): Possible Connections and Clinical Implications

Rusch

Gill

2015

Journal of Clinical Sleep Medicine

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In their letter to the editor published in this issue of Journal of Clinical Sleep Medicine, Dong and Zhang 1 indicate a concern about our study that arises from their own related animal model study. Since the authors did not provide a citation for their associated research, we have limited insight into their perspective. Our study 2 included a cohort of military personnel with a high prevalence of traumatic brain injury (TBI), posttraumatic stress disorder (PTSD), and depression. There are signifi cant challenges and limitations in translating animal models of these complex disorders to the clinical setting. 3Briefl y, neurotrauma models often fail to consider appropriate blast scaling methods and PTSD models have yet to characterize the gestalt of the disorder.3,4 Moreover, genetically homogeneous rodent colonies fail to refl ect the infi nitely varied genotypes of humans that underlie these complex conditions. 5We appreciate the authors highlighting their fi ndings of a weak inverse relationship between decreased expression of insulin-like growth hormone receptor (IGF-1R) and increased concentrations of IGF-1. While this fi nding is interesting, reduced receptor expression doesn't necessarily indicate a reduced signaling capacity. An alternative interpretation may be that the receptor plays a vital role in protein homeostasis and thus there is a slight decrease in IGF-1R in response to the increase in IGF-1 (i.e., a negative feedback mechanism). It is also possible to increase the signaling capacity of a receptor without increasing its quantity, such as in the mechanism of selective serotonin reuptake inhibitors (SSRI). 6,7The authors also state that our paper leads readers to the conclusion that increased concentrations of IGF-1 improve the cognitive functioning of our participants. It's not clear how this conclusion was inferred, as we did not assess a cognitive outcome and explicitly reported that concentration levels of IGF-1 were not associated with a diagnosis of depression, PTSD, or TBI. The current data indicated that IGF-1 concentrations increased in participants who endorsed improved sleep quality following a 12-week sleep intervention, and that improved sleep quality was associated with reductions in depression and posttraumatic arousal symptoms.We agree with the authors that IGF-1 may protect against the effects of stress and that IGF-1 regulates critical hippocampal processes, some of which play a functionally important role in the pathogenesis of PTSD. 8 We echo the author's sentiments that it's not evident from our current study that administration of IGF-1 will improve insomnia or attenuate comorbid symptoms. However, since there was a positive association between sleep quality improvements and IGF-1 increases, which is also confi rmed by a recent Cochrane meta-analysis, 9 it may be a treatment intervention worth exploring. We thank Mr. Dong and Dr. Zhang for taking a special interest in our research and sharing their ideas with us. CITATION

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Section: 7supporting

confidence: 51%

Effect of Acute Sleep Disturbance and Recovery on Insulin-Like Growth Factor-1 (IGF-1): Possible Connections and Clinical Implications

Rusch

Gill

2015

Journal of Clinical Sleep Medicine

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“…Previous functional imaging studies have demonstrated smaller hippocampal volumes in patients with depression and PTSD (Sheline, 2003;Campbell et al, 2004;Bonne et al, 2008;Wang et al, 2010). Hence, we determined whether stress-induced dendritic spine loss might also represent a biological marker for vulnerability to stress.…”

Section: Resultsmentioning

confidence: 94%

“…Individual differences in susceptibility to stress-related cognitive and morphological changes Patients with stress-related psychiatric disorders often display persistent cognitive dysfunction that lasts for many weeks or months after the traumatic event (McNally, 2006;Wang et al, 2010). To characterize the molecular basis of susceptibility and resistance to stress-related psychiatric disorders, we adopted an acute, unpredictable, and inescapable restraint tailshock stress paradigm that profoundly impairs hippocampus-dependent spatial tasks such as object location memory (OLM) in rodents (Howland and Cazakoff, 2010;Roozendaal et al, 2010).…”

Section: Resultsmentioning

confidence: 99%

A Critical Role for Protein Tyrosine Phosphatase Nonreceptor Type 5 in Determining Individual Susceptibility to Develop Stress-Related Cognitive and Morphological Changes

Yang

Huang

2012

J. Neurosci.

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While stressful life events confer increased risk for the development of psychopathology, most individuals experiencing adversity maintain normal psychological functioning, suggesting that individual differences may influence the susceptibility to develop stress-related psychiatric disorders. However, little is known about what determines this difference between individuals at the molecular level. In the present study, we identify that protein tyrosine phosphatase nonreceptor type 5 (PTPN5) (also known as STEP) is a critical determinant of differences in individual susceptibility to develop stress-related cognitive and morphological changes in rats. Our data demonstrate that ablation of PTPN5 expression delays physiological recovery from stress and augments the development of stress-related cognitive and morphological changes, whereas overexpression of a constitutively active variant of PTPN5 enhances the individual's resilience to stress. Our data also reveal that reduced PTPN5 expression prolongs the duration of extracellular signal-regulated kinase activation, leading to an elevation of Ca V 1.2 channel expression and a recovery delay of K V 4.2 channels from inactivation, which in turn heightens neuronal vulnerability to glutamate toxicity. Moreover, intraperitoneal injections of L-type Ca 2ϩ channel blocker nifedipine after stress resulted in a significantly lower rate for developing stress-related cognitive and morphological changes seen in PTPN5 knockdown rats. Together, these results identify a novel role for PTPN5 in mediating the development of stress-related cognitive and morphological changes and suggest that people with PTPN5 deficiency may have a greater susceptibility to capture the deleterious effects of stress.

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“…Neurogenesis impairment has been reported in rodent stress-induced models of depression (Pham et al, 2003) and there are consistent reports of smaller dentate gyrus (DG) and cornu ammonis 3 (CA3) subfield volumes in patients with post-traumatic stress disorder, with sparing of other hippocampal subfields (Wang et al, 2010). Determinants of hippocampal volume in MDD are not known.…”

Section: Introductionmentioning

confidence: 99%

Hippocampal Granule Neuron Number and Dentate Gyrus Volume in Antidepressant-Treated and Untreated Major Depression

Boldrini

Santiago

Hen

et al. 2013

Neuropsychopharmacol

302

210

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Smaller hippocampal volume is reported in major depressive disorder (MDD). We hypothesize that it may be related to fewer granule neurons (GN) in the dentate gyrus (DG), a defect possibly reversible with antidepressants. We studied age-, sex-, and postmortem interval-matched groups: no major psychopathology (controls); unmedicated-MDD; and MDD treated with serotonin reuptake inhibitors (MDD*SSRI) or tricyclics (MDD*TCA). Frozen right hippocampi were fixed, sectioned (50 mm), immunostained with neuronal nuclear marker (NeuN), and counterstained with hematoxylin. GN and glial number, and DG and granule cell layer (GCL) volumes were stereologically estimated. Fewer GNs in the anterior DG were present in unmedicated-MDDs compared with controls (p ¼ 0.013). Younger age of MDD onset correlated with fewer GNs (p ¼ 0.021). Unmedicated-MDDs had fewer mid-DG GNs than MDD*SSRIs (p ¼ 0.028) and controls (p ¼ 0.032). Anterior GCL glial number did not differ between groups. Anterior/mid GCL volume was smaller in unmedicated-MDDs vs controls (p ¼ 0.008) and larger in MDD*SSRIs vs unmedicated-MDDs (po0.001), MDD*TCAs (po0.001), and controls (po0.001). Anterior GCL volume and GN number (r ¼ 0.594, p ¼ 0.001), and mid DG volume and GN number (r ¼ 0.398, p ¼ 0.044) were correlated. Anterior DG capillary density correlated with GN number (p ¼ 0.027), and with GCL (p ¼ 0.024) and DG (r ¼ 0.400, p ¼ 0.047) volumes. Posterior DG volume and GN number did not differ between groups. Fewer GNs in unmedicated-MDD without fewer neuronal progenitor cells, as previously reported, suggests a cell maturation or survival defect, perhaps related to MDD duration. This may contribute to a smaller hippocampus and is potentially reversed by SSRIs. Postmortem studies are correlative and animal studies are needed to test implied causal relationships.

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Magnetic Resonance Imaging of Hippocampal Subfields in Posttraumatic Stress Disorder

Cited by 265 publications

References 63 publications

Effect of Acute Sleep Disturbance and Recovery on Insulin-Like Growth Factor-1 (IGF-1): Possible Connections and Clinical Implications

Effect of Acute Sleep Disturbance and Recovery on Insulin-Like Growth Factor-1 (IGF-1): Possible Connections and Clinical Implications

A Critical Role for Protein Tyrosine Phosphatase Nonreceptor Type 5 in Determining Individual Susceptibility to Develop Stress-Related Cognitive and Morphological Changes

Hippocampal Granule Neuron Number and Dentate Gyrus Volume in Antidepressant-Treated and Untreated Major Depression

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