Neuropathological quantification of dtg APP/PS1: neuroimaging, stereology, and biochemistry

Manaye, Kebreten F.; Wang, Paul; O’Neil, Jahn N.; Huang, Sophia; Xu, Tao; Lei, De-Liang; Tizabi, Yousef; Ottinger, Mary Ann; Ingram, Donald K.; Mouton, Peter R.

doi:10.1007/s11357-007-9035-y

Cited by 35 publications

(26 citation statements)

References 38 publications

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“…Measurements and analyses were performed by an investigator blind to the groups’ identities using the Cavalieri and the Optical Disector/Fractionator and Nucleator methods (Stereo-Investigator; MBF Bioscience, Williston, VT) as previously described (Manaye et al, 2007; Subbiah et al, 1996; West, 1993). The detailed protocols are described in the Supplemental Materials.…”

Section: Methodsmentioning

confidence: 99%

Expression of mutant DISC1 in Purkinje cells increases their spontaneous activity and impairs cognitive and social behaviors in mice

Shevëlkin

Terrillion

Abazyan

et al. 2017

Neurobiology of Disease

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In addition to motor function, the cerebellum has been implicated in cognitive and social behaviors. Various structural and functional abnormalities of Purkinje cells (PCs) have been observed in schizophrenia and autism. As PCs express the gene Disrupted-In-Schizophrenia-1 (DISC1), and DISC1 variants have been associated with neurodevelopmental disorders, we evaluated the role of DISC1 in cerebellar physiology and associated behaviors using a mouse model of inducible and selective expression of a dominant-negative, C-terminus truncated human DISC1 (mutant DISC1) in PCs. Mutant DISC1 male mice demonstrated impaired social and novel placement recognition. No group differences were found in novelty-induced hyperactivity, elevated plus maze test, spontaneous alternation, spatial recognition in Y maze, sociability or accelerated rotarod. Expression of mutant DISC1 was associated with a decreased number of large somata PCs (volume: 3000–5000 μm3) and an increased number of smaller somata PCs (volume: 750–1000 μm3) without affecting the total number of PCs or the volume of the cerebellum. Compared to control mice, attached loose patch recordings of PCs in mutant DISC1 mice revealed increased spontaneous firing of PCs; and whole cell recordings showed increased amplitude and frequency of mEPSCs without significant changes in either Rinput or parallel fiber EPSC paired-pulse ratio. Our findings indicate that mutant DISC1 alters the physiology of PCs, possibly leading to abnormal recognition memory in mice.

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Section: Methodsmentioning

confidence: 99%

Expression of mutant DISC1 in Purkinje cells increases their spontaneous activity and impairs cognitive and social behaviors in mice

Shevëlkin

Terrillion

Abazyan

et al. 2017

Neurobiology of Disease

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“…Increased astroglial responses precede the oxidative impairments of critical cellular components in an AD animal model (Zhu et al 2008). Recent studies have shown that the number of astrocytes is significantly increased in the hippocampus in APP/PS1 mice compared with age-and gender-matched wild-type littermates (Manaye et al 2007). We have previously described that astrocytic gliosis is an early event in the course of APP/PS1-related pathology and that iron administration during the neonatal period and its late effects are independent of the genetic substrate of the individuals, as similar astrocytic responses were observed Fig.…”

Section: Discussionmentioning

confidence: 99%

Early Post-Natal Iron Administration Induces Astroglial Response in the Brain of Adult and Aged Rats

et al. 2010

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This study was aimed to investigate neuropathological changes in adult and aged rats subjected to supplementary iron administration in a critical postnatal period to study the contribution of environmental risk factors to the pathogenesis of neurodegenerative disorders. Ten rats received a single daily oral administration of iron (10 mg/kg) between 12th and 14th post-natal days; nine rats received vehicle (sorbitol 5% in water) in the same period. Five iron-treated and three sorbitol-treated rats were killed at the age of 3 months while five iron-treated and six sorbitol-treated rats were killed at age of 24 months and their brains processed for immunohistochemistry. Increased astrocytosis, revealed by densitometry of GFAP-immunoreactive astrocytes, was found in aged (24 months) iron-treated rats in the substantia nigra and striatum and in the hippocampus of adult (3 months) iron-treated rats when compared to age-matching controls. Decreased densitometry of neurons, revealed by neuronal nucleus immunohistochemistry, was found in aged (24 months) iron-treated rats in substantia nigra and striatum when compared to age-matching controls. These findings suggest that transient dietary iron supplementation during the neonatal period is associated to cellular imprinting in the brain later in life.

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“…Because previous studies have reported increased amyloid load in male dtg AβPP swe /PS1 ΔE9 mice, studies of amyloid load in the present study were limited to the molecular layer in hippocampus of female dtg AβPP swe /PS1 ΔE9 mice. The mean total numbers of pyramidal neurons in CA1 and CA2/3 regions of hippocampus were quantified using the optical fractionator method [49, 50], as previously reported [7, 21, 43, 44, 47, 51–54]. Briefly, the reference spaces on each sampled section were outlined under low power magnification (4X), and volume of Aβ and total number of cells quantified using a high resolution, oil immersion objective (60X, 1.4 numerical aperture).…”

Section: Methodsmentioning

confidence: 99%

“…Sampling of all parameters was continued to a mean coefficient of error (CE) of 0.05 to 0.10, according to Gundersen et al [55]. All stereological parameters were quantified with assistance from a computerized stereology system by an operator blind to treatment and according to established principles, as detailed previously [21, 43, 47, 48, 51]. …”

Section: Methodsmentioning

confidence: 99%

17α-Estradiol Attenuates Neuron Loss in Ovariectomized Dtg AβPP/PS1 Mice

Manaye

Allard

Kalifa

et al. 2011

JAD

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Quantitative microanalysis of brains from patients with Alzheimer's disease (AD) find neuronal loss and neuroinflammation in structures that control cognitive function. Though historically difficult to recapitulate in experimental models, several groups have recently reported that by middle-age, transgenic mice that co-express high levels of two AD-associated mutations, amyloid-β protein precursor (AβPPswe) and presenilin 1 (PS1ΔE9), undergo significant AD-type neuron loss in sub-cortical nuclei with heavy catecholaminergic projections to the hippocampal formation. Here we report that by 13 months of age these dtg AβPPswe/PS1ΔE9 mice also show significant loss of pyramidal neuron in a critical region for learning and memory, the CA1 subregion of hippocampus, as a direct function of amyloid-β (Aβ) aggregation. We used these mice to test whether 17α-estradiol (17αE2), a less feminizing and non-carcinogenic enantiomer of 17β-estradiol, protects against this CA1 neuron loss. Female dtg AβPPswe/PS1ΔE9 mice were ovariectomized at 8–9 months of age and treated for 60 days with either 17αE2 or placebo via subcutaneous pellets. Computerized stereology revealed that 17αE2 ameliorated the loss of neurons in CA1 and reduced microglial activation in the hippocampus. These findings support the view that 17αE2, which may act through non-genomic mechanisms independent of traditional estrogen receptors, could prevent or delay the progression of AD in older men and women.

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Neuropathological quantification of dtg APP/PS1: neuroimaging, stereology, and biochemistry

Cited by 35 publications

References 38 publications

Expression of mutant DISC1 in Purkinje cells increases their spontaneous activity and impairs cognitive and social behaviors in mice

Expression of mutant DISC1 in Purkinje cells increases their spontaneous activity and impairs cognitive and social behaviors in mice

Early Post-Natal Iron Administration Induces Astroglial Response in the Brain of Adult and Aged Rats

17α-Estradiol Attenuates Neuron Loss in Ovariectomized Dtg AβPP/PS1 Mice

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