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Complement C3 Lowering in Adult Inducible Conditional Knockout Mice: Long‐Lasting Effects

Batista, Andre Felipe ; Schroeder, Maren K ; Khan, Khyrul ; [et al.]

Wiley ; 2022

In: Alzheimer's & Dementia Vol. 18, No. S4 ( 2022-12)

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In: Alzheimer's & Dementia, Wiley, Vol. 18, No. S4 ( 2022-12)

Abstract: Complement C3, a central component of the complement cascade, participates in synaptic elimination during brain development and is elevated in the brain with aging and Alzheimer’s disease (AD). Germline C3 knockout (KO) protects against age‐ and AD‐related hippocampal synapse loss and functional decline (Shi Q et al., J Neurosci 2015; Shi Q et al., Sci Transl Med 2017). We crossed C3 fl/fl mice with Rosa26‐Cre‐ERT2 mice to generate global C3 inducible conditional KO mice (C3iKO). Previously, we reported that 5 daily TAM treatments in C3iKO mice at 4‐5 mo of age led to sustained C3 reductions of ∼95% in serum and ∼80% in brain, and protected mice against age‐related cognitive decline at 16‐17 months. In addition, TAM treatment at 3‐4 mo of age protected long‐term potentiation (LTP) in hippocampal slices exposed to toxic Aβ dimers (S26C) obtained at 7‐8 mo of age. Here, we extend our analyses to include changes in complement, cytokine and ApoE expression in these same C3iKO mice and provide confirmatory results in a second cohort of mice. Method qRT‐PCR was used to quantify brain gene expression in the first cohort. In the second cohort, C3iKO, C3 fl/fl and C3KO mice were treated with TAM or corn oil (CO) at 7‐8 mo of age. Cognitive testing commenced at 17‐18 mo and included the Spatial Novelty Y Maze (SPNY), Novel Object Recognition (NOR) and Displaced Object Recognition (DOR). Mice were euthanized and hippocampal synaptosomes isolated for Western blot analysis. Result One‐year post‐treatment, C1qa, C1qb, C1qc, C3, CD11b, CD18, IL‐1β, IFNα, IFNβ, and APOE mRNAs were reduced, and TGFβ and TGFβR1 mRNAs were elevated in brains of TAM‐treated C3iKO and C3KO mice compared to CO‐treated C3iKO mice. In the second cohort, C3 protein levels were reduced ∼92% in serum and ∼77% in hippocampal synaptosomes in TAM‐treated C3iKO mice. TAM‐treated C3iKO mice and both C3KO groups showed significantly better performance in SNYM, LOR and DOR tests compared to controls, consistent with our first study. Pre‐ and post‐synaptic markers were elevated in TAM‐treated vs. CO‐treated C3iKO hippocampal synaptosomes. Conclusion Global C3 lowering in adulthood has long‐lasting effects on immune signaling and hippocampal function. (NIH RF1 AG060057‐CAL)

Type of Medium: Online Resource

ISSN: 1552-5260 , 1552-5279

URL: Issue

URL: Article

DOI: 10.1002/alz.v18.S4

DOI: 10.1002/alz.068094

Language: English

Publisher: Wiley

Publication Date: 2022

detail.hit.zdb_id: 2201940-6

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Global C3 lowering alleviates hippocampal dysfunction and cognitive impairment in aged mice

Batista, Andre Felipe ; Schroeder, Maren K ; Khan, Khyrul ; [et al.]

Wiley ; 2021

In: Alzheimer's & Dementia Vol. 17, No. S2 ( 2021-12)

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In: Alzheimer's & Dementia, Wiley, Vol. 17, No. S2 ( 2021-12)

Abstract: Complement component C3, an innate immune molecule, is important for removing pathogens and eliminating synapses during brain development, aging, and Alzheimer’s disease (AD). Previously, our group demonstrated that C3 deficiency protected against synapse loss during normal aging in wild‐type and APPswe/PS1dE9 mice. Induction of C3 deficiency after normal brain development will help inform whether its inhibition in aging or early stages of AD may serve as a future therapeutic strategy. Method We crossed C3fl/fl mice with an inducible, global Cre line (Rosa26‐Cre‐ERT2+/‐) for 2 generations to generate novel inducible C3 conditional knockout C3fl/fl; Rosa26‐Cre‐ERT2+/‐ mice (C3iKO). In one cohort, four‐to‐five‐month‐old mice were injected with tamoxifen (TAM) or corn oil (CO) daily for 5 days. Behavioral tasks were performed when these mice reached 16‐17 months of age. In another study, three‐to‐four‐month‐old female mice were injected with either CO/TAM and electrophysiological recording of long‐term potentiation (LTP) was conducted in hippocampal slices of TAM‐treated and CO‐treated mice at 7‐8 months of age following incubation of the slices with neurotoxic Aβ S26 dimers. Result C3iKO mice had a significant 85‐95% reduction in serum C3 levels compared to controls, which was consistent at all timepoints analyzed (from Day 7 to Day 365). In this cohort, behavioral testing for hippocampal‐dependent spatial memory, object memory, and object location was performed when TAM‐treated and CO‐treated mice reached 16‐17 months of age. C3iKO+TAM mice performed significantly better than C3iKO+CO‐treated mice in these behavioral tasks, indicating that C3 lowering after brain development protected mice from age‐related cognitive decline. In the second study, we found that C3 lowering in adult mice protected hippocampal synapses from Aβ S26 dimer‐mediated LTP impairment. Conclusion Global C3 depletion in C3iKO young adult mice protected against hippocampal dysfunction as they aged, suggesting that C3 lowering may be an effective therapeutic strategy for aging and possibly, AD. Future studies are underway to investigate the C3‐mediated mechanisms of synaptic dysfunction in the hippocampus.

Type of Medium: Online Resource

ISSN: 1552-5260 , 1552-5279

URL: Issue

URL: Article

DOI: 10.1002/alz.v17.S2

DOI: 10.1002/alz.058736

Language: English

Publisher: Wiley

Publication Date: 2021

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A novel inducible complement C3 conditional knockout mouse model: Generation and characterization : Developing topics

Batista, Andre Felipe ; Schroeder, Maren ; Khan, Khyrul ; [et al.]

Wiley ; 2020

In: Alzheimer's & Dementia Vol. 16, No. S3 ( 2020-12)

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In: Alzheimer's & Dementia, Wiley, Vol. 16, No. S3 ( 2020-12)

Abstract: The classical complement pathway is a complex process involved in the elimination of dead cells, debris, and pathogens, and as well as brain wiring during development. Complement protein C3 is an innate immune molecule central in the complement pathway. It participates in removing pathogens and eliminating synapses, and is elevated with aging and neurodegenerative diseases, including Alzheimer’s Disease. Previously, we showed that lifelong, germline C3‐deficiency protected aged male wild‐type and APPswe/PS1dE9 mice against hippocampal neuronal dysfunction and cognitive decline, despite increasing the Aβ plaque load. However, it remains unknown whether suppressing complement C3 signaling during early stages of AD pathogenesis, when relevant therapeutic interventions might be considered, would confer neuroprotection. Method To address this question, we generated the first‐ever C3 floxed (C3 fl/fl ) mouse line, and then crossed the C3fl/fl mice with an inducible, global Cre line (Rosa26‐Cre‐ERT2 +/‐ ) for 2 generations to generate novel inducible C3 conditional knockout C3 fl/fl ; Rosa26‐Cre‐ERT2 +/‐ mice. Mice aged 2‐3 months received intraperitoneal injections of either corn oil or tamoxifen (75 mg/kg) once a day for 5 consecutive days. We analyzed the C3 serum levels at 7, 14, 30, 60, and 90 days post‐tamoxifen treatment. We also analyzed the mRNA expression of complement C1q and C3 in the brain and liver 60 days following tamoxifen treatment. Result C3 fl/fl ;Rosa26‐cre‐ERT2 +/‐ mice had a significant 70% reduction in serum C3 levels compared to controls, which was consistent at all timepoints analyzed. We also showed that C3 expression in the liver, the main source of complement proteins, as well as in the brain was reduced, demonstrating effective recombinase activity in these organs. Intriguingly, C1q mRNA expression was increased in the brain and liver following tamoxifen treatment; further studies are underway. Conclusion In conclusion, we present a novel mouse model in which tamoxifen treatment resulted in sustained lowering of C3 in the serum, liver, and brain. We will next cross this model with AD‐like mouse models of amyloidosis and tau pathology to evaluate whether global C3 lowering in early stages AD pathogenesis is protective and if so, our data would support targeting complement as a therapy for AD.

Type of Medium: Online Resource

ISSN: 1552-5260 , 1552-5279

URL: Issue

URL: Article

DOI: 10.1002/alz.v16.S3

DOI: 10.1002/alz.047192

Language: English

Publisher: Wiley

Publication Date: 2020

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Therapeutic Efficacy of the Murine Precursor to PBD‐C06: a Novel CDC‐Mutant Anti‐pGlu3Aβ mAb

Bathini, Praveen ; Grenon, Martine ; Papavergi, Maria‐Giusy ; [et al.]

Wiley ; 2022

In: Alzheimer's & Dementia Vol. 18, No. S3 ( 2022-12)

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In: Alzheimer's & Dementia, Wiley, Vol. 18, No. S3 ( 2022-12)

Abstract: Pyroglutamate ‐ 3Aβ (pGlu3Aβ) is a toxic N‐terminally truncated and modified form of Aβ that leads to faster aggregation and seeding of plaques, making it an important target in Alzheimer’s disease. Anti‐amyloid antibodies, e.g., bapineuzumab, are associated with Amyloid‐Related Imaging Abnormalities (ARIA) involving vasogenic edema and microhemorrhages in AD patients, especially in ApoE4 carriers. Previously, we demonstrated reductions in plaques and cognitive deficits using an anti‐pGlu3Ab mAb, 07/2a. Here, we tested a novel CDC‐mutant version (07/2a‐k, murine precursor to PBD‐C06) to avoid C1q activation to reduce vascular‐related inflammation associated with anti‐amyloid antibodies. Method To estimate an effective therapeutic dose, 12 mo‐old APP/PS1dE9 mice were treated weekly (i.p.) for 5 weeks with 150, 300 or 600 µg 07/2a‐k or IgG2a (n=10‐12/group). General Ab and pGlu3Aβ levels were quantified by ELISA and immunohistochemistry. Next, 16 mo‐old APP/PS1dE9; hApoE4 mice were treated weekly (i.p.) for 15 weeks with 350 µg of 07/2a‐k, 3D6‐L (a murine analog of bapineuzumab), or IgG2a, while hApoE4 mice were treated with PBS (n=10‐13 mice/group). Subsequently, cognitive testing was performed over 3 weeks using the Spatial Novelty Y Maze (SNYM), Novel Object Recognition (NOR), and the Barnes Maze followed by euthanasia. Result Five weekly treatments with 07/2a‐k in the dosing study did not alter general and pGlu3 Aβ biochemical levels; however, hippocampal pGlu3Aβ plaques were significantly reduced (300 µg, p 〈 0.0005; 600 µg, p 〈 0.005). In the therapeutic study, 3D6‐L reduced Aβ x‐42 levels (p 〈 0.009) by ELISA but not Ab x‐40 levels. 07/2a‐k did not significantly alter Aβ x‐42 or Ab x‐40 levels. Both antibodies improved performance in the NOR test (07/2a‐k, p 〈 0.05; 3D6‐L, p=0.05) and showed a non‐significant trend for improvement in the SNYM and Barnes maze compared to IgG2a controls. Macro‐hemorrhages were visible in 33% of 3D6‐L treated mice but not in 07/2a‐k treated mice. Conclusion Treatment with the 3D6‐L mAb, a murine analog of bapineuzumab, lowered cerebral Aβ levels and improved cognition but induced macro‐hemorrhages in aged APP/PS1dE9;hApoE4 mice, while treatment with 07/2a‐k, the precursor to PBD‐C06, did not alter general Ab levels but improved cognition in the absence of macro‐hemorrhages. Further analyses are underway to quantify cerebral pGlu3Ab levels, plaques, CAA, microhemorrhages and gliosis. (NIH 1RF1AG058657‐CAL)

Type of Medium: Online Resource

ISSN: 1552-5260 , 1552-5279

URL: Issue

URL: Article

DOI: 10.1002/alz.v18.S3

DOI: 10.1002/alz.067892

Language: English

Publisher: Wiley

Publication Date: 2022

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Temporal Characterization of the Amyloidogenic APP/PS1dE9;hAPOE4 Mouse Model of Alzheimer’s Disease

Grenon, Martine ; Bathini, Praveen ; Papavergi, Maria‐Giusy ; [et al.]

Wiley ; 2022

In: Alzheimer's & Dementia Vol. 18, No. S3 ( 2022-12)

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In: Alzheimer's & Dementia, Wiley, Vol. 18, No. S3 ( 2022-12)

Abstract: The development of immunotherapies against Aβ is burdened by clinical adverse events (AEs) observed as amyloid‐related imaging abnormalities (ARIA) on magnetic resonance imaging scans. The vascular inflammatory AEs have been reported in AD clinical trials administrating certain anti‐Aβ plaque‐binding antibodies and are thought to represent cerebral microhemorrhages and vasogenic edema. ARIA incidence appears apolipoprotein (APOE) genotype‐dependent, wherein APOE E4 allele carriers are at higher risk when compared to non‐carriers. With hopes to robustly model patients most at risk for the vascular complications of anti‐Aβ immunotherapy, we selected a relatively new transgenic mouse model bearing the human APOE E4 gene. The model has not yet been extensively characterized at multiple age points. To assess the face validity of the mouse model, we are conducting a battery of histological and biochemical tests. Methods To evaluate age‐ and sex‐related pathological changes, we collected brain and blood plasma from euthanized male and female APP/PS1dE9;hAPOE4 (APP/E4) mice across 3 ages: 8‐, 12‐ and 16‐months. General‐ and pGlu3‐Aβ levels were quantified using enzyme‐linked immunoassays (ELISA). Prussian Blue hemosiderin staining was used to examine microhemorrhages. Results Immunoassays of brain homogenates exhibited significantly higher insoluble Aβ x‐40 , Aβ x‐42 and pGlu3Aβ levels in 16‐month‐old mice compared to 8‐ and 12‐month‐old mice. Moreover, the 16‐month‐old females demonstrated significantly higher levels of Aβ x‐40 and pGlu3Aβ than age‐matched males. Hemosiderin staining was observed in all 12‐ and 16‐month mice, however no significant differences in abundance was found between the 2 age points. Immunostainings for plaque deposition of various Aβ species, vascular amyloid, dystrophic neurites and gliosis are ongoing. Conclusions Age‐ and sex‐dependent increases in Aβ deposition were revealed in the APP/E4 mouse model. Preliminary evidence for microhemorrhage was observed. Subsequent analyses will better characterize the translational credibility of APP/E4 as a model for future nonclinical immunotherapies targeting Aβ. (1RF1AG058657‐CAL)

Type of Medium: Online Resource

ISSN: 1552-5260 , 1552-5279

URL: Issue

URL: Article

DOI: 10.1002/alz.v18.S3

DOI: 10.1002/alz.067085

Language: English

Publisher: Wiley

Publication Date: 2022

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The Oklahoma City Micronet

Basara, Jeffrey B. ; Illston, Bradley G. ; Fiebrich, Christopher A. ; [et al.]

Wiley ; 2011

In: Meteorological Applications Vol. 18, No. 3 ( 2011-09), p. 252-261

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In: Meteorological Applications, Wiley, Vol. 18, No. 3 ( 2011-09), p. 252-261

Abstract: The Oklahoma City Micronet (OKCNET) is an operational surface observing network designed to improve atmospheric monitoring across the Oklahoma City, Oklahoma, metropolitan area. The 40 station network consists of 4 Oklahoma Mesonet stations and 36 micronet stations mounted on traffic signals at an average station spacing of approximately 3 km. Using several technical innovations as well as existing infrastructure in Oklahoma City, data are collected and quality assured in near real‐time at an interval of 1 min for the traffic signal sites and 5 min for the Mesonet sites. Because OKCNET also spans a land use gradient from rural to urban, the spatial and temporal densities of OKCNET observations have shed new insights on atmospheric processes (e.g. the urban heat island, severe thunderstorm evolution) across the Oklahoma City metropolitan area. Copyright © 2010 Royal Meteorological Society

Type of Medium: Online Resource

ISSN: 1350-4827 , 1469-8080

URL: Issue

URL: Article

DOI: 10.1002/met.v18.3

DOI: 10.1002/met.189

Language: English

Publisher: Wiley

Publication Date: 2011

detail.hit.zdb_id: 1482937-X

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Relation between smoking cessation and receiving results from three annual spiral chest computed tomography scans for lung carcinoma screening

Townsend, Cynthia O. ; Clark, Matthew M. ; Jett, James R. ; [et al.]

Wiley ; 2005

In: Cancer Vol. 103, No. 10 ( 2005-05-15), p. 2154-2162

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In: Cancer, Wiley, Vol. 103, No. 10 ( 2005-05-15), p. 2154-2162

Type of Medium: Online Resource

ISSN: 0008-543X , 1097-0142

URL: Issue

URL: Journal

URL: Article

DOI: 10.1002/cncr.v103:10

DOI: 10.1002/(ISSN)1097-0142

DOI: 10.1002/cncr.21045

Language: English

Publisher: Wiley

Publication Date: 2005

detail.hit.zdb_id: 1479932-7

detail.hit.zdb_id: 2599218-1

detail.hit.zdb_id: 2594979-2

detail.hit.zdb_id: 1429-1

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