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EditorialEDITORIAL

Exceeding the Limits of the Normal Blood-Brain Barrier: Quo Vadis Gadolinium?

L.M. Levy
American Journal of Neuroradiology November 2007, 28 (10) 1835-1836; DOI: https://doi.org/10.3174/ajnr.A0725
L.M. Levy
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In this issue of the American Journal of Neuroradiology, hyperintense CSF in the subarachnoid space is demonstrated on fluid-attenuated inversion recovery (FLAIR) imaging in patients who had gadolinium-enhanced MR imaging (Morris et al). These surprising findings are described in subjects without abnormalities known to disrupt the blood-brain barrier and can occur with or without the presence of renal insufficiency.

Although this finding is reversible and may represent a diagnostic pitfall, there can be important implications. Clinical issues such as drug dosage and administration, toxicity, and contraindications need to be carefully considered. New and useful pathophysiologic information may be obtained from the imaging findings. Mechanisms involving the behavior of the normal and abnormal blood-brain barrier may be further clarified.

Whether gadolinium contrast enters the CSF is presently not in question. In studies of healthy animals and in vitro phantoms, Mamourian et al1 showed that gadolinium concentration in CSF increased with the administered dose of contrast. The in vitro gadolinium effects were observable on FLAIR images at concentrations 4 times lower than those on T1-weighted images. The amount of visualized CSF signal-intensity change should depend on technical factors such as the dose of contrast, injection speed, and pressure; however, the presence of underlying clinical conditions may also exacerbate this effect. Although the severity of the underlying barrier disruption and the resulting clinical consequences are not fully known, similar CSF signal-intensity changes have been observed with major disruptions of the blood-brain barrier in studies involving neurologic disorders such as ischemic stroke, epilepsy, tumors, and acute brain injuries. In a study of seizures, the high CSF signal intensity on sequential FLAIR images was attributed to high protein levels in CSF, secondary to disruptions of the blood-brain barrier related to seizure activity.2 More specifically, blood-brain barrier leakage may occur during epileptogenesis and the chronic epileptic phase, contributing to the progression of epilepsy.3 If free gadolinium is actually released from the chelated complexes, significant neurotoxicity may then occur. Predisposing conditions such as renal dysfunction may lead to elevated free gadolinium in the CSF. In fact, subacute encephalopathy secondary to inadvertent repetitive gadolinium contrast administration did occur in a patient in renal failure.4 Although this type of complication could be reduced with proper hemodialysis, intrathecal gadolinium has been shown to produce movement disorders and ataxia in animals, with necrosis and myelinolysis. More generally, the phenomenon of CSF signal-intensity change is not just limited to gadolinium because similar results have been observed with iodinated contrast injection. In a series involving patients with acute ischemia treated with intra-arterial thrombolysis, Kim et al5 noted that sulcal hyperintensity on FLAIR imaging may be caused by iodinated contrast medium. Again, this should not be considered subarachnoid hemorrhage and could be associated with subsequent hemorrhagic transformation.

Where does the leakage actually occur? Presently, the physiologic mechanisms that control the brain environment are collectively known as the blood-brain barrier and consist of an anatomic barrier and a regulatory interface.6 In the early 1900s, it was observed that dyes injected into the circulation did not stain the CSF, and this led to the idea of a blood-brain barrier. However, the typical morphologic features of the blood-brain barrier are not present in all brain regions. The first component of the blood-brain barrier occurs at the cerebral microvasculature level and is composed of unique cerebral capillary endothelial cells with tight junctions. The lack of permeability of this barrier and the absence of intraparenchymal enhancement on postcontrast scans suggest that it is an unlikely pathway for gadolinium penetration.

A second component is the blood-CSF barrier at the choroid plexus level, first demonstrated by Goldmann in 1913 and further analyzed by Broman in 1941.6 The blood-CSF barrier is essential in maintaining homeostasis and in the regulating neuronal function. Unlike the blood-brain barrier, the blood-CSF barrier is selectively permeable and therefore could have allowed the passage of gadolinium under certain conditions.

A third component consists of the circumventricular organs, several small regions including the neurohypophysis, median eminence, pineal gland, supraoptic crest, area postrema, and the subfornical and subcomissural organs. Because the blood vessels in the circumventricular organs have increased permeability compared with those in other brain regions, they can allow the free passage of gadolinium. However, the surface area of the circumventricular organs is 5000 times smaller than the blood-brain barrier, compared with either the surface areas of the blood-CSF or blood-brain barriers, which are both of the same order of magnitude. It is thus unlikely that the relative contribution of the circumventricular organs to CSF signal-intensity change is significant, though the effects of regionally increased gadolinium leakage remain unclear. In the future, detailed imaging could perhaps resolve the sites of leakage more accurately.

Although there has been significant research regarding the blood-brain barrier, the mechanisms involving its function and the consequences of its dysfunction are still under investigation. However, present studies indicate that a damaged blood-brain barrier may allow toxins to enter the brain, leading to neurologic conditions, including epilepsy, inflammation, and Alzheimer disease.7

With the continued development of improved imaging techniques, there is now an increasing need to evaluate the significance and consequences of greater intravenous contrast use. Our advances in imaging should also lead to a better understanding of the mechanisms underlying blood-brain barrier abnormalities.

References

  1. ↵
    Mamourian AC, Hoopes PJ, Lewis LD. Visualization of intravenously administered contrast material in the CSF on fluid-attenuated inversion-recovery MR images: an in vitro and animal-model investigation. AJNR Am J Neuroradiol 2000;21:105–11
    Abstract/FREE Full Text
  2. ↵
    Villalobos-Chavez F, Rodriguez-Uranga JJ, Sanz-Fernandez G. Sequential changes in magnetic resonance in a limbic status epilepticus [in Spanish]. Rev Neurol 2005;40:354–57
    PubMed
  3. ↵
    van Vliet EA, da Costa Arauji S, Redeker S, et al. Blood-brain barrier leakage may lead to progression of temporal lobe epilepsy. Brain 2007;130(Pt 2):521–34. Epub 2006 Nov 22
  4. ↵
    Maramattom BV, Manno Em, Wijdicks EF, et al. Gadolinium encephalopathy in a patient with renal failure. Neurology 2005;64:1276–78
    Abstract/FREE Full Text
  5. ↵
    Kim EY, Kim SS, Na DG, et al. Sulcal hyperintensity on fluid-attenuated inversion recovery imaging in acute ischemic stroke patients treated with intra-arterial thrombolysis: iodinated contrast media as its possible cause and the association with hemorrhagic transformation. J Comput Assist Tomogr 2005;29:264–69
    CrossRefPubMed
  6. ↵
    Levy LM. What is right about MRI permeability studies. AJNR Am J Neuroradiol 2005;26:3–4
    FREE Full Text
  7. ↵
    Pluta R. Is the ischemic blood-brain barrier insufficiency responsible for full-blown Alzheimer’s disease? Neurol Res 2006;28:665–71
    CrossRefPubMed
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American Journal of Neuroradiology: 28 (10)
American Journal of Neuroradiology
Vol. 28, Issue 10
November 2007
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Exceeding the Limits of the Normal Blood-Brain Barrier: Quo Vadis Gadolinium?
L.M. Levy
American Journal of Neuroradiology Nov 2007, 28 (10) 1835-1836; DOI: 10.3174/ajnr.A0725

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Exceeding the Limits of the Normal Blood-Brain Barrier: Quo Vadis Gadolinium?
L.M. Levy
American Journal of Neuroradiology Nov 2007, 28 (10) 1835-1836; DOI: 10.3174/ajnr.A0725
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