Biologic Nanoparticles and Platelet Reactivity

Miller, Virginia M.; Hunter, Larry W.; Chu, Kevin; Kaul, Vivasvat; Squillace, Phillip D; Lieske, John C.; Jayachandran, Muthuvel

doi:10.2217/nnm.09.61

Cited by 33 publications

(19 citation statements)

References 37 publications

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“…Previous studies suggested that natural hydroxyapatite particles from human calcified tissue may interfere with platelet aggregation [30][31][32]. In the present study it was shown that doped and nondoped HAP nanoparticles did not interfere with the coagulation pathway up to a concentration of 250 mg/mL.…”

Section: Platelet Adhesion and Activationsupporting

confidence: 52%

Different hydroxyapatite magnetic nanoparticles for medical imaging: Its effects on hemostatic, hemolytic activity and cellular cytotoxicity

Laranjeira

Moço

Ferreira

et al. 2016

Colloids and Surfaces B: Biointerfaces

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Section: Platelet Adhesion and Activationsupporting

confidence: 52%

Different hydroxyapatite magnetic nanoparticles for medical imaging: Its effects on hemostatic, hemolytic activity and cellular cytotoxicity

Laranjeira

Moço

Ferreira

et al. 2016

Colloids and Surfaces B: Biointerfaces

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“…For instance, multi walled carbon nanotubes (MWNT) and single walled carbon nanotubes (SWNT) induce platelet aggregation, but not activation [58]. Contrary to that, biological NPs (hydroxyapetite-HA and calcified NP) inhibited platelet aggregation but induced activation [59]. A similar observation was made for TiO 2 NPs [60].…”

Section: Thrombocytes/plateletsmentioning

confidence: 62%

Blood protein and blood cell interactions with gold nanoparticles: the need for in vivo studies

Shah

Bischof²

2013

BioNanoMaterials

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Gold nanoparticles (GNPs) have gained in prominence within the field of nanomedicine with recent advancement of several embodiments to clinical trials. To ensure their success in the clinic it has become increasingly clear that a deeper understanding of the biological interactions of GNPs is imperative. Since the majority of GNPs are intended for systemic intravenous use, an immediate and critical biological interaction is between the blood and the GNP. Blood is composed of plasma proteins and cells. Both of these components can induce downstream effects upon interacting with GNPs that ultimately influence their medical impact. For instance, proteins from the blood can cover the GNP to create a biological identity through formation of a protein corona that is quite different from the originally synthesized GNP. Once in the bloodstream this protein coated GNP evokes both positive and negative physiological responses such as biodistribution into tissue for therapy (i.e., cancer) and toxicity or off target accumulation in the reticuloendothelial system (RES) that must be controlled for optimal use. In this review, we summarize predominantly in vitro studies of GNP interactions with blood plasma proteins and blood cells and make the case that more in vivo study is urgently needed to optimal design and control GNP use in medicine. In some cases where no specific GNP blood studies exist, we draw the readers ' attention to studies conducted with other types of nanoparticles as reference.

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“…Women randomized to active treatments also received oral progesterone (Prometrium; micronized progesterone, 200 mg/day) for 12 days each month for the duration of the study to protect the uterus. Each participant underwent a medical examination, including body morphometrics and standard blood chemistries prior to randomization 19, 22 .…”

Section: Methodsmentioning

confidence: 99%

Differential effects of hormone therapy on serotonin, vascular function and mood in the KEEPS

et al. 2015

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Background Serotonin (5-hydroxytryptamine, 5-HT) is modulated by sex steroid hormones and affects vascular function and mood. In the Kronos Early Estrogen Prevention Cognitive and Affective Ancillary Study (KEEPS-Cog), women randomized to oral conjugated equine estrogens (oCEE) showed greater benefit on affective mood states than women randomized to transdermal 17β-estradiol (tE2) or placebo (PL). This study examined the effect of these treatments on the platelet content of 5-HT as a surrogate measure of 5-HT synthesis and uptake in the brain. Methods The following were measured in a subset (n = 79) of women enrolled in KEEPS-Cog: 5-HT by ELISA, carotid intima-medial thickness (CIMT) by ultrasound, endothelial function by reactive hyperemia index (RHI), and self-reported symptoms of affective mood states by the Profile of Mood States (POMS) questionnaire. Results Mean platelet content of 5-HT increased by 107.0%, 84.5% and 39.8%, in tE2, oCEE and PL groups, respectively. Platelet 5-HT positively correlated with estrone in the oCEE group and with 17β- estradiol in the tE2 group. Platelet 5-HT showed a positive association with RHI, but not CIMT, in the PL and oCEE groups. Reduction in mood scores for depression-dejection and anger-hostility associated with elevations in platelet 5-HT only in the oCEE group (r = −0.5, p = 0.02). Conclusions Effects of oCEE compared to tE2 on RHI and mood may be related to mechanisms involving platelet, and perhaps neuronal, uptake and release of 5-HT and reflect conversion of estrone to bioavailable 17β- estradiol in platelets and the brain.

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Biologic Nanoparticles and Platelet Reactivity

Cited by 33 publications

References 37 publications

Different hydroxyapatite magnetic nanoparticles for medical imaging: Its effects on hemostatic, hemolytic activity and cellular cytotoxicity

Different hydroxyapatite magnetic nanoparticles for medical imaging: Its effects on hemostatic, hemolytic activity and cellular cytotoxicity

Blood protein and blood cell interactions with gold nanoparticles: the need for in vivo studies

Differential effects of hormone therapy on serotonin, vascular function and mood in the KEEPS

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