Contrast enhanced X-ray computed tomography imaging of amyloid plaques in Alzheimer disease rat model on lab based micro CT system

Kavková, Michaela; Zikmund, Tomáš; Kala, Annu; Šalplachta, Jakub; Pena, Stephanie L. Proskauer; Kaiser, Jozef; Jezek, Karel

doi:10.1038/s41598-021-84579-x

Cited by 15 publications

(19 citation statements)

References 41 publications

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“…The rat model TgF-344 AD is built on a platform of Fisher-344 phenotype, by inserting the human mutated genes for amyloid precursor protein APP ("Swedish" mutation, APPsw) and ∆ exon 9 presenilin-1 PS1 ∆ E9AβPP [11]. The subjects show a formation of amyloid beta deposits, tangles of hyper-phosphorylated Tau, neurodegeneration and cognitive impairment [11][12][13][14].…”

Section: Introductionmentioning

confidence: 99%

Early Spatial Memory Impairment in a Double Transgenic Model of Alzheimer’s Disease TgF-344 AD

et al. 2021

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Before the course of Alzheimer’s disease fully manifests itself and largely impairs a patient’s cognitive abilities, its progression has already lasted for a considerable time without being noticed. In this project, we mapped the development of spatial orientation impairment in an active place avoidance task—a highly sensitive test for mild hippocampal damage. We tested vision, anxiety and spatial orientation performance at four age levels of 4, 6, 9, and 12 months across male and female TgF-344 AD rats carrying human genes for presenilin-1 and amyloid precursor protein. We found a progressive deterioration of spatial navigation in transgenic animals, beginning already at the age of 4 months, that fully developed at 6 months of age across both male and female groups, compared to their age-matched controls. In addition, we described the gradual vision impairment that was accentuated in females at the age of 12 months. These results indicate a rather early onset of cognitive impairment in the TgF-344 AD Alzheimer’s disease model, starting earlier than shown to date, and preceding the reported development of amyloid plaques.

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Section: Introductionmentioning

confidence: 99%

Early Spatial Memory Impairment in a Double Transgenic Model of Alzheimer’s Disease TgF-344 AD

et al. 2021

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“…Our study is focused on ex vivo evaluation of tissues’ properties, as Xradia Versa 520 unit is not supposed for in vivo studies. There are micro‐CT systems designed for rat and mice studies, which inquire contrast‐enhanced 3D visualization structural changes of inner organs 45–47 . It should be noted that the capabilities of these systems for visualization in large magnification are several times lower than ex vivo micro‐CT systems, which results in less detailed 3D reconstruction.…”

Section: Discussionmentioning

confidence: 99%

X‐ray micro‐computed tomography in the assessment of penile cavernous fibrosis in a rabbit castration model

et al. 2021

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Background: Current assessment methods of penile cavernous fibrosis in animal models have limitations due to the inability to provide complex and volume analysis of fibrotic alterations. Objective:The aim was to evaluate micro-computed tomography for assessment of cavernous fibrosis and compare it with histological, histochemical, immunohistochemical, and RT-PCR analysis. Materials and methods:A controlled trial was performed involving 25 New Zealand male rabbits with induced testosterone deficiency by orchidectomy. Penile samples were obtained before and after 7, 14, 21, and 84 days from orchidectomy. We consistently performed (a) gray value analysis of corpora cavernosa 3D models reconstructed after micro-computed tomography, (b) morphometry of smooth muscles/connective tissue ratio, collagen type I/III ratio, and area of TGF-beta-1 expression in corpora cavernosa, and (c) RT-PCR of TGF-beta-1 expression.Results: Micro-computed tomography allowed visualization of penile structures at a resolution comparable to light microscopy. Gray values of corpora cavernosa decreased from 1673 (1512-1773) on the initial day to 1184 (1089-1232) on the 21st day (p < 0.005). However, on the 84th day, it increased to 1610 (1551-1768). On 21st and 84th days, there was observed a significant decrease in smooth muscle/connective tissue ratio and a significant increase in collagen type I/III ratio (p < 0.05). TGF-beta1 expression increased on the 84th day according to immunohistochemistry (p < 0.005).RT-PCR was impossible to conduct due to the absence of RNA in obtained samples after micro-CT.Discussion and conclusions: Micro-computed tomography provided 3D visualization of entire corpora cavernosa and assessment of radiodensity alterations by gray value

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“…The staining of soft tissues with ionic contrast agents has been used for imaging in the micro-CT of brain 37 and whole-body 38 of zebra sh, as well as, rodent embryos, brains and other organs 29,28,38 . Some have even gone further, staining whole mice brains to identify/quantify electrode lesions 39 , tumours 40 , malformations 41 , disease pathology in Alzheimer's 42 and even single neurons 43 44 . Nevertheless, the use of these stains for the visualization and quanti cation of cerebrovascular alterations 45 and ischemic lesion 16,46,47,48 in whole mouse brains have rarely been described and never with great tissue/lesion contrast.…”

Section: Introductionmentioning

confidence: 99%

“…This is a particularly di cult task in the segmentation of speci c brain structures, due to the low contrast offered by different types of tissue and anatomical structures. Manual segmentation, where a skilled operator delineates the structures of interest by hand, is thus still popular in the segmentation of micro-CT images of the brain, due to its accuracy and low requirements 16,42 . However, it's major disadvantage is the high time-cost, which poses a signi cant bottleneck in the whole analysis pipeline.…”

Section: Introductionmentioning

confidence: 99%

High resolution micro-CT imaging in mice stroke models: from 3D detailed infarct characterization to automatic area segmentation

Gomes

Pinto

Matula

et al. 2022

Preprint

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Characterization of brain infarct lesion in rodent models of stroke is crucial to assess the outcome of stroke therapies and to study the disease pathophysiology. However, so far it has been mostly performed by: 1) histological methods, a time-consuming process that lead to significant flaws; or 2) via MRI imaging, which is faster, yielding 3D information but at high costs. High-resolution micro-CT imaging became, in the last decade, a simple, fast, and cheaper solution, allowing 3D sample analysis. Here, we describe that high-resolution micro-CT, either using iodine/OsO4 as contrast agents, can be successfully applied for fine quantification and localization of lesion size and edema volume in preclinical stroke models. We successfully correlated this new approach with the standard histological method TTC. In transient MCAO mouse stroke model, we were able to identify/quantify large lesioned areas (segmented in core/penumbra), up to degenerated finer striatal myelinated fibers in a transient-ischemic-attack (TIA) mouse model, at different timepoints post-ischemia, through manual/automatic segmentation approaches (deep learning). Furthermore, whole brain 3D reconstructions allow brain atlas co-registration with specific affected brain areas. Hence, the presented methodology, through iodine/OsO4 micro-CT imaging, constitutes a valuable advance for precise and detailed assessment of stroke outcomes in preclinical animal studies.

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Contrast enhanced X-ray computed tomography imaging of amyloid plaques in Alzheimer disease rat model on lab based micro CT system

Cited by 15 publications

References 41 publications

Early Spatial Memory Impairment in a Double Transgenic Model of Alzheimer’s Disease TgF-344 AD

Early Spatial Memory Impairment in a Double Transgenic Model of Alzheimer’s Disease TgF-344 AD

X‐ray micro‐computed tomography in the assessment of penile cavernous fibrosis in a rabbit castration model

High resolution micro-CT imaging in mice stroke models: from 3D detailed infarct characterization to automatic area segmentation

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