Distribution of Glycylsarcosine and Cefadroxil among Cerebrospinal Fluid, Choroid Plexus, and Brain Parenchyma after Intracerebroventricular Injection is Markedly Different between Wild-Type and Pept2 Null Mice

David E Smith; Yongjun Hu; Hong Shen; Tavarekere N Nagaraja; Joseph D Fenstermacher; Richard F Keep

doi:10.1038/jcbfm.2010.84

Distribution of Glycylsarcosine and Cefadroxil among Cerebrospinal Fluid, Choroid Plexus, and Brain Parenchyma after Intracerebroventricular Injection is Markedly Different between Wild-Type and Pept2 Null Mice

Journal of Cerebral Blood Flow & Metabolism ◽

10.1038/jcbfm.2010.84 ◽

2010 ◽

Vol 31 (1) ◽

pp. 250-261 ◽

Cited By ~ 22

Author(s):

David E Smith ◽

Yongjun Hu ◽

Hong Shen ◽

Tavarekere N Nagaraja ◽

Joseph D Fenstermacher ◽

...

Keyword(s):

Cerebrospinal Fluid ◽

Choroid Plexus ◽

Interstitial Fluid ◽

Brain Parenchyma ◽

Wild Type ◽

Septal Region ◽

Biodistribution Studies ◽

Choroid Plexuses ◽

Clearance Kinetics ◽

The Brain

The purpose of this study was to define the cerebrospinal fluid (CSF) clearance kinetics, choroid plexus uptake, and parenchymal penetration of PEPT2 substrates in different regions of the brain after intracerebroventricular administration. To accomplish these objectives, we performed biodistribution studies using [14C]glycylsarcosine (GlySar) and [3H]cefadroxil, along with quantitative autoradiography of [14C]GlySar, in wild-type and Pept2 null mice. We found that PEPT2 deletion markedly reduced the uptake of GlySar and cefadroxil in choroid plexuses at 60 mins by 94% and 82% ( P<0.001), respectively, and lowered their CSF clearances by about fourfold. Autoradiography showed that GlySar concentrations in the lateral, third, and fourth ventricle choroid plexuses were higher in wild-type as compared with Pept2 null mice ( P<0.01). Uptake of GlySar by the ependymal–subependymal layer and septal region was higher in wild-type than in null mice, but the half-distance of penetration into parenchyma was significantly less in wild-type mice. The latter is probably because of the clearance of GlySar from interstitial fluid by brain cells expressing PEPT2, which stops further penetration. These studies show that PEPT2 knockout can significantly modify the spatial distribution of GlySar and cefadroxil (and presumably other peptides/mimetics and peptide-like drugs) in brain.

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Distribution of Suramin, an Antitrypanosomal Drug, across the Blood-Brain and Blood-Cerebrospinal Fluid Interfaces in Wild-Type and P-Glycoprotein Transporter-Deficient Mice

Antimicrobial Agents and Chemotherapy ◽

10.1128/aac.00372-07 ◽

2007 ◽

Vol 51 (9) ◽

pp. 3136-3146 ◽

Cited By ~ 25

Author(s):

Lisa Sanderson ◽

Adil Khan ◽

Sarah Thomas

Keyword(s):

Choroid Plexus ◽

Brain Perfusion ◽

Brain Parenchyma ◽

Sleeping Sickness ◽

New Drugs ◽

Wild Type ◽

P Glycoprotein ◽

Blood Brain ◽

Targeted Mutation ◽

The Brain

ABSTRACT Although 60 million people are exposed to human African trypanosomiasis, drug companies have not been interested in developing new drugs due to the lack of financial reward. No new drugs will be available for several years. A clearer understanding of the distribution of existing drugs into the brains of sleeping sickness patients is needed if we are to use the treatments that are available more safely and effectively. This proposal addresses this issue by using established animal models. Using in situ brain perfusion and isolated incubated choroid plexus techniques, we investigated the distribution of [3H]suramin into the central nervous systems (CNSs) of male BALB/c, FVB (wild-type), and P-glycoprotein-deficient (Mdr1a/Mdr1b-targeted mutation) mice. There was no difference in the [3H]suramin distributions between the three strains of mice. [3H]suramin had a distribution similar to that of the vascular marker, [14C]sucrose, into the regions of the brain parenchyma that have a blood-brain barrier. However, the association of [3H]suramin with the circumventricular organ samples, including the choroid plexus, was higher than that of [14C]sucrose. The association of [3H]suramin with the choroid plexus was also sensitive to phenylarsine oxide, an inhibitor of endocytosis. The distribution of [3H]suramin to the brain was not affected by the presence of other antitrypanosomal drugs or the P-glycoprotein efflux transporter. Overall, the results confirm that [3H]suramin would be unlikely to treat the second or CNS stage of sleeping sickness.

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Cerebrospinal Fluid and Interstitial Fluid Motion via the Glymphatic Pathway Modelled by Optimal Mass Transport

10.1101/043281 ◽

2016 ◽

Cited By ~ 1

Author(s):

Vadim Ratner ◽

Yi Gao ◽

Hedok Lee ◽

Maikan Nedergaard ◽

Helene Benveniste ◽

...

Keyword(s):

Cerebrospinal Fluid ◽

Interstitial Fluid ◽

Initial Conditions ◽

Fluid Motion ◽

Flow Patterns ◽

Brain Parenchyma ◽

Fluid Exchange ◽

Waste Products ◽

Glymphatic Pathway ◽

The Brain

It was recently shown that the brain-wide cerebrospinal fluid (CSF) and interstitial fluid exchange system designated the `glymphatic pathway' plays a key role in removing waste products from the brain, similarly to the lymphatic system in other body organs [1,2]. It is therefore important to study the flow patterns of glymphatic transport through the live brain in order to better understand its functionality in normal and pathological states. Unlike blood, the CSF does not flow rapidly through a network of dedicated vessels, but rather through peri-vascular channels and brain parenchyma in a slower time-domain, and thus conventional fMRI or other blood-flow sensitive MRI sequences do not provide much useful information about the desired flow patterns. We have accordingly analyzed a series of MRI images, taken at different times, of the brain of a live rat, which was injected with a paramagnetic tracer into the CSF via the lumbar intrathecal space of the spine. Our goal is twofold: (a) find glymphatic (tracer) flow directions in the live rodent brain; and (b) provide a model of a (healthy) brain that will allow the prediction of tracer concentrations given initial conditions. We model the liquid flow through the brain by the diffusion equation. We then use the Optimal Mass Transfer (OMT) approach [3] to model the glymphatic flow vector field, and estimate the diffusion tensors by analyzing the (changes in the) flow. Simulations show that the resulting model successfully reproduces the dominant features of the experimental data.

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Epithelial Pathways in Choroid Plexus Electrolyte Transport

Physiology ◽

10.1152/physiol.00011.2010 ◽

2010 ◽

Vol 25 (4) ◽

pp. 239-249 ◽

Cited By ~ 38

Author(s):

Helle H. Damkier ◽

Peter D. Brown ◽

Jeppe Praetorius

Keyword(s):

Cerebrospinal Fluid ◽

Chemical Composition ◽

Choroid Plexus ◽

Interstitial Fluid ◽

Electrolyte Transport ◽

Molecular Pathways ◽

Choroid Plexus Epithelium ◽

Neuronal Function ◽

The Brain

A stable intraventricular milieu is crucial for maintaining normal neuronal function. The choroid plexus epithelium produces the cerebrospinal fluid and in doing so influences the chemical composition of the interstitial fluid of the brain. Here, we review the molecular pathways involved in transport of the electrolytes Na+, K+, Cl−, and HCO3− across the choroid plexus epithelium.

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Kinetic Profile of the Transcriptome Changes Induced in the Choroid Plexus by Peripheral Inflammation

Journal of Cerebral Blood Flow & Metabolism ◽

10.1038/jcbfm.2009.15 ◽

2009 ◽

Vol 29 (5) ◽

pp. 921-932 ◽

Cited By ~ 62

Author(s):

Fernanda Marques ◽

João C Sousa ◽

Giovanni Coppola ◽

Ana M Falcao ◽

Ana João Rodrigues ◽

...

Keyword(s):

Cerebrospinal Fluid ◽

Choroid Plexus ◽

Acute Phase ◽

Acute Phase Proteins ◽

Brain Parenchyma ◽

Matrix Remodeling ◽

Choroid Plexus Epithelial Cell ◽

Blood Concentrations ◽

The Brain

The choroid plexus, being part of the blood-brain barriers and responsible for the production of cerebrospinal fluid, is ideally positioned to transmit signals into and out of the brain. This study, using microarray analysis, shows that the mouse choroid plexus displays an acute-phase response after an inflammatory stimulus induced in the periphery by lipopolysaccharide (LPS). Remarkably, the response is specific to a restricted number of genes (out of a total of 24,000 genes analyzed, 252 are up-regulated and 173 are down-regulated) and transient, as it returns to basal conditions within 72 h. The up-regulated genes cluster into families implicated in immune-mediated cascades and in extracellular matrix remodeling, whereas those down-regulated participate in maintenance of the barrier function. Importantly, several acute-phase proteins, whose blood concentrations rise in response to inflammation, may contribute to the effects observed in vivo after LPS injection, as suggested by the differential response of primary choroid plexus epithelial cell cultures to LPS alone or to serum collected from animals exposed to LPS. By modulating the composition of the cerebrospinal fluid, which will ultimately influence the brain parenchyma, the choroid plexus response to inflammation may be of relevance in brain homeostasis in health and disease.

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Transthyretin is not essential for thyroxine to reach the brain and other tissues in transthyretin-null mice

AJP Endocrinology and Metabolism ◽

10.1152/ajpendo.1997.272.3.e485 ◽

1997 ◽

Vol 272 (3) ◽

pp. E485-E493 ◽

Cited By ~ 7

Author(s):

J. A. Palha ◽

M. T. Hays ◽

G. Morreale de Escobar ◽

V. Episkopou ◽

M. E. Gottesman ◽

...

Keyword(s):

Cerebrospinal Fluid ◽

Choroid Plexus ◽

Null Mouse ◽

Tissue Uptake ◽

Wild Type ◽

Transfer Rates ◽

Physiological Conditions ◽

Liver And Kidney ◽

The Brain ◽

Brain Barriers

As part of a study on tissue uptake of thyroxine (T4) in a transthyretin (TTR)-null mouse strain, kinetic parameters of thyroxine metabolism in wild-type mice under normal physiological conditions are presented. Kinetic analysis of injected [(125)I]T4 showed that TTR-null mutants have markedly increased [(125)I]T4 transfer rate constants from plasma to the fast-exchange compartments of liver and kidney and from fast to slow kidney compartments. Transfer rates from plasma to brain, testes, and fat were little affected. The T4 tissue content in the mutants was greatly reduced in brain but relatively normal in liver and kidney. No major changes were observed in brain 3,3',5-triiodothyronine concentrations, suggesting that availability of this hormone is not markedly altered in the mutant mice. The low T4 brain content probably reflects the absence of T4-TTR complexes in the mutant choroid plexus and cerebrospinal fluid. This study indicates that TTR is not essential for T4 tissue uptake or for T4 to reach the brain across the choroid plexus-cerebrospinal fluid and/or blood-brain barriers.

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Choroid plexus glutathione peroxidases are instrumental in protecting the brain fluid environment from hydroperoxides during postnatal development

AJP Cell Physiology ◽

10.1152/ajpcell.00094.2018 ◽

2018 ◽

Vol 315 (4) ◽

pp. C445-C456 ◽

Cited By ~ 3

Author(s):

Elodie Saudrais ◽

Nathalie Strazielle ◽

Jean-François Ghersi-Egea

Keyword(s):

Cerebrospinal Fluid ◽

Choroid Plexus ◽

Neurological Impairment ◽

Physiological Concentration ◽

Cell Network ◽

Glutathione Peroxidases ◽

Choroid Plexuses ◽

Fluid Environment ◽

The Brain

Hydrogen peroxide, released at low physiological concentration, is involved in different cell signaling pathways during brain development. When released at supraphysiological concentrations in brain fluids following an inflammatory, hypoxic, or toxic stress, it can initiate lipid peroxidation, protein, and nucleic acid damage and contribute to long-term neurological impairment associated with perinatal diseases. We found high glutathione peroxidase and glutathione reductase enzymatic activities in both lateral and fourth ventricle choroid plexus tissue isolated from developing rats, in comparison to the cerebral cortex and liver. Consistent with these, a high protein expression of glutathione peroxidases 1 and 4 was observed in choroid plexus epithelial cells, which form the blood-cerebrospinal fluid barrier. Live choroid plexuses isolated from newborn rats were highly efficient in detoxifying H2O2 from mock cerebrospinal fluid, illustrating the capacity of the choroid plexuses to control H2O2 concentration in the ventricular system of the brain. We used a differentiated cellular model of the blood-cerebrospinal fluid barrier coupled to kinetic and inhibition analyses to show that glutathione peroxidases are more potent than catalase to detoxify extracellular H2O2 at concentrations up to 250 µM. The choroidal cells also formed an enzymatic barrier preventing blood-borne hydroperoxides to reach the cerebrospinal fluid. These data point out the choroid plexuses as key structures in the control of hydroperoxide levels in the cerebral fluid environment during development, at a time when the protective glial cell network is still immature. Glutathione peroxidases are the main effectors of this choroidal hydroperoxide inactivation.

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Thiamine transport in the central nervous system

American Journal of Physiology-Legacy Content ◽

10.1152/ajplegacy.1976.230.4.1101 ◽

1976 ◽

Vol 230 (4) ◽

pp. 1101-1107 ◽

Cited By ~ 39

Author(s):

R Spector

Keyword(s):

Choroid Plexus ◽

Intraventricular Injection ◽

Simple Diffusion ◽

Thiamine Transport ◽

Choroid Plexuses ◽

The Central Nervous System ◽

The Brain ◽

Thiamine Phosphates

Total thiamine (free thiamine and thiamine phosphates) transport into the cerebrospinal fluid (CSF), brain, and choroid plexus and out of the CSF was measured in rabbits. In vivo, total thiamine transport into CSF, choroid plexus, and brain was saturable. At the normal plasma total thiamine concentration, less than 5% of total thiamine entry into CSF, choroid plexus, and brain was by simple diffusion. The relative turnovers of total thiamine in choroid plexus, whole brain, and CSF were 5, 2, and 14% per h, respectively, when measured by the penetration of 35S-labeled thiamine injected into blood. From the CSF, clearance of [35S]thiamine relative to mannitol was not saturable after the intraventricular injection of various concentrations of thiamine. However, a portion of the [35S]thiamine cleared from the CSF entered brain by a saturable mechanism. In vitro, choroid plexuses, isolated from rabbits and incubated in artificial CSF, accumulated [35S]thiamine against a concentration gradient by an active saturable process that did not depend on pyrophosphorylation of the [35S]thiamine. The [35S]thiamine accumulated within the choroid plexus in vitro was readily released. These results were interpreted as showing that the entry of total thiamine into the brain and CSF from blood is regulated by a saturable transport system, and that the locus of this system may be, in part, in the choroid plexus.

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The Potential Roles of Blood–Brain Barrier and Blood–Cerebrospinal Fluid Barrier in Maintaining Brain Manganese Homeostasis

Nutrients ◽

10.3390/nu13061833 ◽

2021 ◽

Vol 13 (6) ◽

pp. 1833

Author(s):

Shannon Morgan McCabe ◽

Ningning Zhao

Keyword(s):

Cerebrospinal Fluid ◽

Blood Brain Barrier ◽

Blood Circulation ◽

Critical Role ◽

Systemic Circulation ◽

Brain Parenchyma ◽

Brain Barrier ◽

Blood Brain ◽

The Brain

Manganese (Mn) is a trace nutrient necessary for life but becomes neurotoxic at high concentrations in the brain. The brain is a “privileged” organ that is separated from systemic blood circulation mainly by two barriers. Endothelial cells within the brain form tight junctions and act as the blood–brain barrier (BBB), which physically separates circulating blood from the brain parenchyma. Between the blood and the cerebrospinal fluid (CSF) is the choroid plexus (CP), which is a tissue that acts as the blood–CSF barrier (BCB). Pharmaceuticals, proteins, and metals in the systemic circulation are unable to reach the brain and spinal cord unless transported through either of the two brain barriers. The BBB and the BCB consist of tightly connected cells that fulfill the critical role of neuroprotection and control the exchange of materials between the brain environment and blood circulation. Many recent publications provide insights into Mn transport in vivo or in cell models. In this review, we will focus on the current research regarding Mn metabolism in the brain and discuss the potential roles of the BBB and BCB in maintaining brain Mn homeostasis.

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Analysis of Changes in Signal Intensity of Choroid Plexus in MRI Using FLAIR-DW-EPI Pulse Sequence

ScholarGen Publishers ◽

10.31916/sjmi2020-01-02 ◽

2020 ◽

Vol 3 (1) ◽

pp. 9-15

Author(s):

Jingyu Kim ◽

◽

Sang-Jin Im ◽

Keyword(s):

Choroid Plexus ◽

Signal Intensity ◽

Pulse Sequence ◽

Signal Strength ◽

Brain Parenchyma ◽

Weighted Image ◽

Diffusion Weighted ◽

Water Signal ◽

The Brain ◽

Functional Problems

In this study, the signal intensity of choroid plexus, which is producing cerebrospinal fluid, is analyzed according to the FLAIR diffusion-weighted imaging technique. In the T2*-DW-EPI diffusion-weighted image, the FLAIR-DW-EPI technique, which suppressed the water signal, was additionally examined for subjects with high choroid plexus signals and compared and analyzed the signal intensity. As a result of the experiment, it was confirmed that the FLAIR-DW-EPI technique showed a signal strength equal to or lower than that of the brain parenchyma, and there was a difference in signal strength between the two techniques. As a result of this study, if the choroidal plexus signal is high in the T2 * -DW-EPI diffusionweighted image, additional examination of the FLAIR-DW-EPI technique is thought to be useful in distinguishing functional problems of the choroid plexus. In conclusion, if the choroidal plexus signal is high on the T2*-DW-EPI diffuse weighted image, it is thought that further examination of the FLAIR-DW-EPI technique will be useful in distinguishing functional problems of the choroidal plexus.

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On the anatomic relation of choroid plexus to brain: a comparative study

AJP Regulatory Integrative and Comparative Physiology ◽

10.1152/ajpregu.1980.238.1.r76 ◽

1980 ◽

Vol 238 (1) ◽

pp. R76-R81 ◽

Cited By ~ 2

Author(s):

H. F. Cserr ◽

M. Bundgaard ◽

J. K. Ashby ◽

M. Murray

Keyword(s):

Choroid Plexus ◽

Brain Volume ◽

Brain Size ◽

Ventricular Volume ◽

Brain Weight ◽

Air Breathing ◽

Original Proposal ◽

Adaptive Value ◽

Choroid Plexuses ◽

The Brain

The size of choroid plexuses and cerebral ventricles relative to brain varies widely among vertebrates. The functional significance of this variability has attracted little attention since Herrick's original proposal that large choroid plexuses might enhance oxygen delivery to the brain and therefore be of adaptive value in the transition of vertebrates from water to air breathing. We compared choroid plexus and brain weight or ventricular and brain volume in 40 species from nine vertebrate groups. Both choroid plexus weight and ventricular volume were unrelated to brain size. Plexus weight ranged from 0 to 5.2% of brain weight and ventricular volume from 0.9 to 132% of brain volume. Amid this diversity the dipnoans, chondrosteans, holosteans, amphibians, and crossopterygian examined in this study are exceptional in uniformly having large plexuses. The adaptive significance of large choroid plexuses may lie in the presence of specific homeostatic mechanisms and their role in the response to the increases in PCO2 that accompany the transition to air breathing.

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