Literature DB >> 28353217

Hypoxic Stress and Inflammatory Pain Disrupt Blood-Brain Barrier Tight Junctions: Implications for Drug Delivery to the Central Nervous System.

Jeffrey J Lochhead1, Patrick T Ronaldson1, Thomas P Davis2.   

Abstract

A functional blood-brain barrier (BBB) is necessary to maintain central nervous system (CNS) homeostasis. Many diseases affecting the CNS, however, alter the functional integrity of the BBB. It has been shown that various diseases and physiological stressors can impact the BBB's ability to selectively restrict passage of substances from the blood to the brain. Modifications of the BBB's permeability properties can potentially contribute to the pathophysiology of CNS diseases and result in altered brain delivery of therapeutic agents. Hypoxia and/or inflammation are central components of a number of diseases affecting the CNS. A number of studies indicate hypoxia or inflammatory pain increase BBB paracellular permeability, induce changes in the expression and/or localization of tight junction proteins, and affect CNS drug uptake. In this review, we look at what is currently known with regard to BBB disruption following a hypoxic or inflammatory insult in vivo. Potential mechanisms involved in altering tight junction components at the BBB are also discussed. A more detailed understanding of the mediators involved in changing BBB functional integrity in response to hypoxia or inflammatory pain could potentially lead to new treatments for CNS diseases with hypoxic or inflammatory components. Additionally, greater insight into the mechanisms involved in TJ rearrangement at the BBB may lead to novel strategies to pharmacologically increase delivery of drugs to the CNS.

Entities:  

Keywords:  blood-brain barrier; drug delivery; hypoxia; pain; tight junctions

Mesh:

Year:  2017        PMID: 28353217      PMCID: PMC5481481          DOI: 10.1208/s12248-017-0076-6

Source DB:  PubMed          Journal:  AAPS J        ISSN: 1550-7416            Impact factor:   4.009


  109 in total

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Review 3.  Physiology of blood-brain interfaces in relation to brain disposition of small compounds and macromolecules.

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4.  Microglial interleukin-1β in the ipsilateral dorsal horn inhibits the development of mirror-image contralateral mechanical allodynia through astrocyte activation in a rat model of inflammatory pain.

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Journal:  Pain       Date:  2015-06       Impact factor: 6.961

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Authors:  Limin Wu; Mohammad R Islam; Janice Lee; Hajime Takase; Shuzhen Guo; Allison M Andrews; Tetyana P Buzhdygan; Justin Mathew; Wenlu Li; Ken Arai; Eng H Lo; Servio H Ramirez; Josephine Lok
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Review 7.  The physiological functions of central nervous system pericytes and a potential role in pain.

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Journal:  F1000Res       Date:  2018-03-20

Review 8.  [Research progress on the effects of plateau hypoxia on blood-brain barrier structure and drug permeability].

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