To evaluate the role of cannabinoid signaling during the comorbidity of HIV and Alzheimer�s disease in the context of HIV-associated cognitive disorders

项目来源

美国卫生和人类服务部基金(HHS)

项目主持人

TSAI, SHANG-YI ANNE

项目受资助机构

Florida International University

立项年度

2019

立项时间

未公开

项目编号

3R01DA040537-05S1

项目级别

国家级

研究期限

未知 / 未知

受资助金额

364031.00美元

学科

Acquired Cognitive Impairment; Aging; Alzheimer's Disease; Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD); Bioengineering; Brain Disorders; Cannabinoid Research; Dementia; Endocannabinoid System Research; Infectious Diseases; Nanotechnology; Neurodegenerative; Neurosciences; Therapeutic Cannabinoid Research;

学科代码

未公开

基金类别

Non-SBIR/STTR RPGs

关键词

未公开

参与者

NAIR, MADHAVAN P.

参与机构

NATIONAL INSTITUTE ON DRUG ABUSE

项目标书摘要:PROJECT SUMMARY of the administrative supplement The objectives of the parent R01 grant are 1) to develop and evaluate the transport, delivery, release on demand and efficacy of nanoformulation containing cannabinoid receptor modulators to activate latent HIV infection, eradicate HIV and protect from HIV/cannabinoid-induced neuronal deficits using an in-vitro BBB-HIV infection cannabinoid model, 2) to evaluate the in vivo efficacy of the developed nanocarrier in HIVE SCID cannabinoid mouse model, and 3) to monitor the neurobehavioral modulations induced by nanoformulation in HIVE SCID cannabinoid mouse model. Thus the three major focuses in the parent R01 are the HIV, magneto- electric nanoparticle (MENP)-based drug delivery and the cannabinoid pathway. Here we want to broaden the scope of these three major focuses by also evaluating the potential of cannabinoid system for therapy during the comorbidity of HIV and Alzheimer?s disease (AD) which is emerging as a major health problem in recent years. Following the introduction of HAART, many HIV patients live longer and thus enter an age when the risk of developing AD increases exponentially. So far, the apoE4 allele is the strongest genetic risk factor identified in sporadic AD patients, and there is also a strong association between apoE4 and the rate of HIV-1 disease progression, suggesting a strong relationship between HIV infection and AD pathogenesis. This is not surprising given the fact that exposure to HIV particles and HIV proteins can directly or indirectly modulate the amyloid and Tau proteins, the two hallmark features of AD. Also, HIV-infected elders have a higher rate of meeting criteria for mild cognitive impairment (MCI). Therefore, we hypothesize a synergistic effect of the comorbidity of HIV and AD on the common neuropathological features such as A?, tau, neurodegeneration, and synaptic loss. Further, treatment with cannabinoid activators through the developed nanoformulation will mitigate these neuropathological features. We will test this hypothesis by generating 3xTg-AD/iTAT bigenic mice (+/- doxycycline) and compare the results with 3xTg-AD and iTAT (+/- Dox) single transgenic lines. In specific aim 1, using MENP technology, we will evaluate the role of cannabinoid CB1 and CB2 receptor agonists and antagonists on the subventricular zone (SVZ) and subgranular zone (SGZ) adult neurogenesis as well as levels of A? and hyperphosphorylated tau. In the specific aim 2, we will evaluate the role of ECS on the dendritic spine density and number of synapses and correlate with learning and memory skills. Since we plan to test the cannabinoid system directly in a mouse model of HIV (iTAT) and AD (3xTg-AD) and address three key questions in HIV/AD research, i.e., HIV and AD comorbidity, cannabinoid multitarget pathway and efficient brain penetration, this administrative supplement request is directly related to Alzheimer?s disease and related dementias (ADRD). If the liposomal-MENP drug delivery in this HIV/AD comorbidity mouse model is successful, it may also be extended to other neurological diseases in future studies.

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  • 2.Anti-inflammatory effects of CBD in human microglial cell line infected with HIV-1.

    • Yndart Arias, Adriana;Kolishetti, Nagesh;Vashist, Arti;Madepalli, Lakshmana;Llaguno, Lorgeleys;Nair, Madhavan
    • 《Scientific reports》
    • 2023年
    • 13卷
    • 1期
    • 期刊

    Human immunodeficiency virus (HIV) infection is associated with a chronic inflammatory stage and continuous activation of inflammasome pathway. We studied the anti-inflammatory effects of the compound cannabidiol (CBD) in comparison with Delta (9)-tetrahydrocannabinol [Delta(9)-THC] in human microglial cells (HC69.5) infected with HIV. Our results showed that CBD reduced the production of various inflammatory cytokines and chemokines such as MIF, SERPIN E1, IL-6, IL-8, GM-CSF, MCP-1, CXCL1, CXCL10, and IL-1 beta compared to Delta(9)-THC treatment. In addition, CBD led to the deactivation of caspase 1, reduced NLRP3 gene expression which play a crucial role in the inflammasome cascade. Furthermore, CBD significantly reduced the expression of HIV. Our study demonstrated that CBD has anti-inflammatory properties and exhibits significant therapeutic potential against HIV-1 infections and neuroinflammation. © 2023. This is a U.S. Government work and not under copyright protection in the US; foreign copyright protection may apply.

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  • 3.Magneto-plasmonic nanostars for image-guided and NIR-triggered drug delivery

    • 关键词:
    • IRON-OXIDE NANOPARTICLES; GOLD NANOPARTICLES; CONTRAST AGENTS; MRI;RESONANCES; THERAPY; CELLS; CORE
    • Tomitaka, Asahi;Arami, Hamed;Ahmadivand, Arash;Pala, Nezih;McGoron, Anthony J.;Takemura, Yasushi;Febo, Marcelo;Nair, Madhavan
    • 《SCIENTIFIC REPORTS》
    • 2020年
    • 10卷
    • 1期
    • 期刊

    Smart multifunctional nanoparticles with magnetic and plasmonic properties assembled on a single nanoplatform are promising for various biomedical applications. Owing to their expanding imaging and therapeutic capabilities in response to external stimuli, they have been explored for on-demand drug delivery, image-guided drug delivery, and simultaneous diagnostic and therapeutic (i.e. theranostic) applications. In this study, we engineered nanoparticles with unique morphology consisting of a superparamagnetic iron oxide core and star-shaped plasmonic shell with high-aspect-ratio gold branches. Strong magnetic and near-infrared (NIR)-responsive plasmonic properties of the engineered nanostars enabled multimodal quantitative imaging combining advantageous functions of magnetic resonance imaging (MRI), magnetic particle imaging (MPI), photoacoustic imaging (PAI), and image-guided drug delivery with a tunable drug release capacity. The model drug molecules bound to the core-shell nanostars were released upon NIR illumination due to the heat generation from the core-shell nanostars. Moreover, our simulation analysis showed that the specific design of the core-shell nanostars demonstrated a pronounced multipolar plasmon resonance, which has not been observed in previous reports. The multimodal imaging and NIR-triggered drug release capabilities of the proposed nanoplatform verify their potential for precise and controllable drug release with different applications in personalized medicine.

    ...
  • 4.Development of Multifunctional Biopolymeric Auto-Fluorescent Micro- and Nanogels as a Platform for Biomedical Applications

    • 关键词:
    • Emulsion polymerization;Biopolymers;Fluorescence;Controlled drug delivery;Emulsions;Nanostructured materials;Emulsification;Biocompatibility;Gels;Targeted drug delivery;Biomedical applications;Blood-brain barrier;Central nervous systems;Hydrogel particles;Hydroxyethyl celluloses (HEC);Image guided therapy;Safe delivery systems;Sustainable resources
    • Vashist, Arti;Atluri, Venkata;Raymond, Andrea;Kaushik, Ajeet;Parira, Tiyash;Huang, Zaohua;Durygin, Andriy;Tomitaka, Asahi;Nikkhah-Moshaie, Roozbeh;Vashist, Atul;Agudelo, Marisela;Chand, Hitendra S.;Saytashev, Ilyas;Ramella-Roman, Jessica C.;Nair, Madhavan
    • 《Frontiers in Bioengineering and Biotechnology》
    • 2020年
    • 8卷
    • 期刊

    The emerging field of theranostics for advanced healthcare has raised the demand for effective and safe delivery systems consisting of therapeutics and diagnostics agents in a single monarchy. This requires the development of multi-functional bio-polymeric systems for efficient image-guided therapeutics. This study reports the development of size-controlled (micro-to-nano) auto-fluorescent biopolymeric hydrogel particles of chitosan and hydroxyethyl cellulose (HEC) synthesized using water-in-oil emulsion polymerization technique. Sustainable resource linseed oil-based polyol is introduced as an element of hydrophobicity with an aim to facilitate their ability to traverse the blood-brain barrier (BBB). These nanogels are demonstrated to have salient features such as biocompatibility, stability, high cellular uptake by a variety of host cells, and ability to transmigrate across an in vitro BBB model. Interestingly, these unique nanogel particles exhibited auto-fluorescence at a wide range of wavelengths 450–780 nm on excitation at 405 nm whereas excitation at 710 nm gives emission at 810 nm. In conclusion, this study proposes the developed bio-polymeric fluorescent micro- and nano- gels as a potential theranostic tool for central nervous system (CNS) drug delivery and image-guided therapy. © Copyright © 2020 Vashist, Atluri, Raymond, Kaushik, Parira, Huang, Durygin, Tomitaka, Nikkhah-Moshaie, Vashist, Agudelo, Chand, Saytashev, Ramella-Roman and Nair.

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  • 5.Dynamic magnetic characterization and magnetic particle imaging enhancement of magnetic-gold core-shell nanoparticles

    • 关键词:
    • ANISOTROPY; NANOTHERANOSTICS; DELIVERY; THERAPY; SIZE
    • Tomitaka, Asahi;Ota, Satoshi;Nishimoto, Kizuku;Arami, Hamed;Takemura, Yasushi;Nair, Madhavan
    • 《NANOSCALE》
    • 2019年
    • 11卷
    • 13期
    • 期刊

    Multifunctional nanoparticles with a magnetic core and gold shell structures are emerging multi-modal imaging probes for disease diagnosis, image-guided therapy, and theranostic applications. Owing to their multi-functional magnetic and plasmonic properties, these nanoparticles can be used as contrast agents in multiple complementary imaging modalities. Magnetic particle imaging (MPI) is a new pre-clinical imaging system that enables real-time imaging with high sensitivity and spatial resolution by detecting the dynamic responses of nanoparticle tracers. In this study, we evaluated the dynamic magnetic properties and MPI imaging performances of core-shell nanoparticles with a magnetic core coated with a gold shell. A change in AC hysteresis loops was detected before and after the formation of the gold shell on magnetic core nanoparticles, suggesting the influence of the core-shell interfacial effect on their dynamic magnetic properties. This alteration in the dynamic responses resulted in an enhancement of the MPI imaging capacity of magnetic nanoparticles. The gold shell coating also enabled a simple and effective functionalization of the nanoparticles with a brain glioma targeting ligand. The enhanced MPI imaging capacity and effective functionality suggest the potential application of the magnetic-gold core-shell nanoparticles for MPI disease diagnostics.

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  • 6.Magnetically guided non-invasive CRISPR-Cas9/gRNA delivery across blood-brain barrier to eradicate latent HIV-1 infection

    • 关键词:
    • RAMAN-SPECTROSCOPY
    • Kaushik, Ajeet;Yndart, Adriana;Atluri, Venkata;Tiwari, Sneham;Tomitaka, Asahi;Gupta, Purnima;Jayant, Rahul Dev;Alvarez-Carbonell, David;Khalili, Kamel;Nair, Madhavan
    • 《SCIENTIFIC REPORTS》
    • 2019年
    • 9卷
    • 期刊

    CRISPR-Cas9/gRNA exhibits therapeutic efficacy against latent human immunodeficiency virus (HIV) genome but the delivery of this therapeutic cargo to the brain remains as a challenge. In this research, for the first time, we demonstrated magnetically guided non-invasive delivery of a nano-formulation (NF), composed of Cas9/gRNA bound with magneto-electric nanoparticles (MENPs), across the blood-brain barrier (BBB) to inhibit latent HIV-1 infection in microglial (h mu glia)/HIV (HC69) cells. An optimized ac-magnetic field of 60 Oe was applied on NF to release Cas9/gRNA from MENPs surface and to facilitate NF cell uptake resulting in intracellular release and inhibition of HIV. The outcomes suggested that developed NF reduced HIV-LTR expression significantly in comparison to unbound Cas9/gRNA in HIV latent h mu glia/HIV (HC69) cells. These findings were also validated qualitatively using fluorescence microscopy to assess NF efficacy against latent HIV in the microglia cells. We believe that CNS delivery of NF (CRISPR/Cas9-gRNA-MENPs) across the BBB certainly will have clinical utility as future personalized nanomedicine to manage neuroHIV/AIDS.

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  • 7.Surface-engineered multimodal magnetic nanoparticles to manage CNS diseases

    • 关键词:
    • IRON-OXIDE NANOPARTICLES; BLOOD-BRAIN-BARRIER; DRUG-DELIVERY;FUNCTIONALIZED NANOPARTICLES; AMYLOID PLAQUES; GLIOBLASTOMA; CELLS;MODEL; HYPERTHERMIA; MAGNETOSOMES

    Advanced central nervous system (CNS) therapies exhibited high efficacy but complete treatment of CNS diseases remains challenging owing to limited delivery of therapeutic agents to the brain. Multifunctional magnetic nanoparticles are investigated not only for site-specific drug delivery but also for theranostic applications aiming for an effective CNS therapy. Recently, surface engineering of magnetic nanoparticles was recognized as a crucial area of research to achieve precise therapy and imaging at molecular and cellular levels. This review reports state-of-the-art advancement in the development of surface-engineered magnetic nanoparticles targeting CNS diagnostics and therapies. The challenges and future prospects of magnetic theranostics are also discussed by considering the translation from bench to bedside. Successful translation of magnetic theranostics to the clinical setting will enable precise and efficient diagnostics and therapy to manage CNS diseases.

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  • 8.MRI-Guided, Noninvasive Delivery of Magneto-Electric Drug Nanocarriers to the Brain in a Nonhuman Primate

    • 关键词:
    • Medical nanotechnology;Targeted drug delivery;Biocompatibility;Brain mapping;Magnetos;Nanomagnetics;Nanoparticles;Noninvasive medical procedures;Controlled drug delivery;Mammals;Brain delivery;Brain image analysis;Central nervous systems;Clinical application;Nano-carriers;Non-human primate;Noninvasive methods;Personalized nanomedicine
    • Kaushik, Ajeet;Rodriguez, Jose;Rothen, Dan;Bhardwaj, Vinay;Jayant, Rahul Dev;Pattany, Pradip;Fuentes, Beatriz;Chand, Hitendra;Kolishetti, Nagesh;El-Hage, Nazira;Khalili, Kamel;Kenyon, Norma S.;Nair, Madhavan
    • 《ACS Applied Bio Materials》
    • 2019年
    • 2卷
    • 11期
    • 期刊

    A magnetically guided brain delivery method previously demonstrated in mice has not yet been translated for clinical applications due to the mismatch of available static magnet dimensions in relation to the human brain size and shape. To develop a human-compatible methodology, we explored magnetic resonance imaging (MRI) as a tool for the delivery of magneto-electric nanoparticles (MENPs) into the brain of a baboon, as a proof-of-concept study. MRI brain image analysis showed a reduction in T2∗ value at the basal ganglia, hemisphere, and vertex, thereby confirming successful MENP delivery to the brain. The observation of well-integrated morphologically healthy tissues and no blood toxicity over the study duration confirmed the biocompatibility of MENPs and the delivery procedure. Outcomes of this research present MRI-assisted delivery of MENPs to the brain as a safe and noninvasive method in larger species such as baboons and one step closer to human translation. This MENP-based nanomedicine delivery method can be used for clinical application in order to investigate effective central nervous system (CNS) therapies. © 2019 American Chemical Society.

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  • 9.Blood-brain barrier pericytes as a target for HIV-1 infection

    • 关键词:
    • blood-brain barrier pericytes; HIV; HIV reservoirs; neuroinfection;HIV-associated neurocognitive disorder;VASCULAR SMOOTH-MUSCLE; IMMUNODEFICIENCY-VIRUS TYPE-1;CENTRAL-NERVOUS-SYSTEM; NEUROVASCULAR UNIT; ENDOTHELIAL-CELLS; NEURALCREST; N-CADHERIN; INTEGRITY; HEALTH; MESOTHELIUM
    • Bertrand, Luc;Cho, Hyung Joon;Toborek, Michal
    • 《BRAIN》
    • 2019年
    • 142卷
    • 期刊

    Pericytes are multifunctional cells wrapped around endothelial cells via cytoplasmic processes that extend along the abluminal surface of the endothelium. The interactions between endothelial cells and pericytes of the blood-brain barrier are necessary for proper formation, development, stabilization, and maintenance of the blood-brain barrier. Blood-brain barrier pericytes regulate paracellular flow between cells, transendothelial fluid transport, maintain optimal chemical composition of the surrounding micro-environment, and protect endothelial cells from potential harmful substances. Thus, dysfunction or loss of blood-brain barrier pericytes is an important factor in the pathogenesis of several diseases that are associated with microvascular instability. Importantly, recent research indicates that blood-brain barrier pericytes can be a target of HIV-1 infection able to support productive HIV-1 replication. In addition, blood-brain barrier pericytes are prone to establish a latent infection, which can be reactivated by a mixture of histone deacetylase inhibitors in combination with TNF. HIV-1 infection of blood-brain barrier pericytes has been confirmed in a mouse model of HIV-1 infection and in human post-mortem samples of HIV-1-infected brains. Overall, recent evidence indicates that blood-brain barrier pericytes can be a previously unrecognized HIV-1 target and reservoir in the brain.

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  • 10.Targeted Mitochondrial COQ(10) Delivery Attenuates Antiretroviral-Drug-Induced Senescence of Neural Progenitor Cells

    • 关键词:
    • aging; antiretroviral therapy; CoQ(10); HIV; mitochondria; oxidativestress; progenitor cells;TENOFOVIR DISOPROXIL FUMARATE; COGNITIVE IMPAIRMENT; OXIDATIVE STRESS;STEM-CELLS; HIV; THERAPY; BRAIN; AGE; INFECTION; SUPPLEMENTATION
    • Velichkovska, Martina;Surnar, Bapurao;Nair, Madhavan;Dhar, Shanta;Toborek, Michal
    • 《MOLECULAR PHARMACEUTICS》
    • 2019年
    • 16卷
    • 2期
    • 期刊

    HIV infection is associated with symptoms of accelerated or accentuated aging that are likely to be driven not only by HIV itself but also by the toxicity of long-term use of antiretroviral drugs. Therefore, it is crucially important to understand the mechanisms by which antiretroviral drugs may contribute to aging. The aim of this study was to investigate the hypothesis that antiretroviral drugs cause increased reactive oxygen species (ROS) generation that results in mitochondrial dysfunction and culminates in promoting cellular senescence. In addition, we applied targeted nano particle (NP)-based delivery to specifically enrich mitochondria with coenzyme Q(10) (CoQ(10)) in order to enhance antioxidant protection. The studies employed neural progenitor cells (NPCs), as differentiation of these cells into mature neurons is affected both during HIV infection and in the aging process. Exposure of cultured NPCs to various combinations of HIV antiretroviral therapy (ART) induced a more than 2-fold increase in mitochondrial ROS generation and mitochondrial membrane potential, a more than 50% decrease in oxygen consumption and ATP levels, a 60% decrease in SIRT3 expression, and a 42% decrease in cell proliferation relative to control levels. These alterations were accompanied by a 37% increase in beta-galactosidase staining and a shortening of the telomere length to more than half of the length of controls as assessed by quantitative telomere-FISH labeling, indicating accelerated NPC senescence in response to ART exposure. Importantly, CoQ(10) delivered by targeted nanoparticles effectively attenuated these effects. Overall, these results indicate that ART promotes cellular senescence by causing mitochondrial dysfunction, which can be successfully reversed by supplementation with mitochondria-targeted CoQ(10).

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