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Cerebral small vessel disease

Last revised by Rohit Sharma on 23 Mar 2024

Citation, DOI, disclosures and article data

Citation:

Weerakkody Y, Sharma R, Deng F, et al. Cerebral small vessel disease. Reference article, Radiopaedia.org (Accessed on 19 Apr 2024) https://doi.org/10.53347/rID-16200

DOI:

https://doi.org/10.53347/rID-16200

Permalink:

https://radiopaedia.org/articles/16200

rID:

16200

Article created:

29 Dec 2011, Yuranga Weerakkody ◉

Disclosures:

At the time the article was created Yuranga Weerakkody had no recorded disclosures.

View Yuranga Weerakkody's current disclosures

Last revised:

23 Mar 2024, Rohit Sharma ◉

Disclosures:

At the time the article was last revised Rohit Sharma had no financial relationships to ineligible companies to disclose.

View Rohit Sharma's current disclosures

Revisions:

25 times, by 12 contributors - see full revision history and disclosures

Systems:

Central Nervous System

Synonyms:

Age-related white matter disease
Ischemic demyelination
Small vessel disease
Deep white matter ischaemia
Microangiopathic leukoencephalopathy
Age-related demyelination
Small vessel ischemic changes
Small vessel chronic ischaemia
Chronic small vessel ischaemic disease
White matter microangiopathy
White matter hyperintensities
White matter lesions
Unidentified bright objects (UBOs)
Unidentified bright object (UBO)
Subcortical small vessel disease
Cerebral microangiopathy
Chronic small vessel disease
White matter disease
Leukoaraiosis

Cerebral small vessel disease, also known as cerebral microangiopathy, is an umbrella term for lesions in the brain attributed to pathology of small arteries, arterioles, capillaries, venules, or small veins. It is the most common cause of vascular dementia/cognitive impairment and is a major cause of ischemic and hemorrhagic strokes.

With respect to anatomy, small vessels include small arteries, arterioles, capillaries, venules, and small veins. The arterial bed has been a primary focus of the literature, with arterial small vessel disease being a proposed term for this entity, but venous collagenosis is also responsible for some of the changes ¹⁵. The small vessels involved are too small to visualize by imaging in vivo, so imaging focuses on their sequelae.

With respect to morphologic changes visible on imaging, small vessel disease includes small subcortical (lacunar) infarcts (of deep gray nuclei and deep white matter), hemorrhages, perivascular spaces, and diffuse white matter changes ^14,16. The latter has received much attention in particular and is largely the focus of this article. Analogous signal changes in the subcortical gray matter and brainstem are typically excluded from discussion unless explicitly stated, leading to terms that focus on small vessel disease of white matter ¹⁶.

The term leukoaraiosis is a radiological descriptor applied to white matter hypodensities on CT and high signal changes on T2-weighted MRI of presumed vascular origin ^14,16. These lesions are also called white matter lesions, white matter hyperintensities (for MRI), or white matter changes ¹⁶. Similar terms focused on the white matter include white matter disease, white matter damage, and leukoencephalopathy (the latter usually used in the context of CADASIL) ¹⁶. Less commonly, the lesions are called unidentified bright objects on MRI, but this term has also confusingly been used to refer to the focal areas of signal intensity in brains of children with neurofibromatosis type 1, which is an unrelated process.

Many etiopathogenic types of small vessel disease are described (see below). The most common is arteriolosclerosis, or age and vascular risk factor related small vessel disease, which based on a progressive clinical syndrome of cognitive impairment and compatible imaging features is diagnosed as Binswanger disease ¹⁴, although this term has fallen in popularity. Many variant terms for this entity presume an age-related etiology, such as age-related white matter hyperintensities/changes/disease/damage ¹⁶, although noting that not all age-related white matter changes are attributed to small vessel disease ¹⁴.

The nature of infarcts and white matter changes are primarily ischemic, so other terms used include small vessel chronic ischemia, microvascular ischemia, ischemic microangiopathy, and variants of the above terms such as ischemic white matter disease. However, hemorrhagic manifestations of small vessel disease (cerebral microbleeds, intracerebral hemorrhage, and cortical superficial siderosis) are also important to consider for differential diagnosis and therapeutic reasons ^15,16.

Epidemiology

Chronic small vessel disease is more common with increasing age. The prevalence of white matter lesions in the general population is reported to be between 39 to 96% ¹¹.

Clinical presentation

Chronic small vessel disease is often an incidental asymptomatic finding on imaging. However, it has been shown to cause vascular dementia and it is more common in patients with dementia (vascular dementia, Alzheimer disease, Lewy body dementia) compared to the general population (100% v. 92% respectively in one study) ^11,12.

Pathology

Etiology

There are several aetiopathogenic types of cerebral small vessel diseases ¹⁵:

arteriolosclerosis (age-related and vascular risk factor-related small vessel disease): see Binswanger disease
cerebral amyloid angiopathy (sporadic or hereditary)
inherited/genetic small vessel diseases other than cerebral amyloid angiopathy, such as
inflammatory and immunologically mediated small vessel diseases (CNS vasculitis)
venous collagenosis
other small vessel diseases, such as
- post-radiation angiopathy
- non-amyloid microvessel degeneration in Alzheimer disease

Microscopic appearance

Histology from these lesions shows atrophy of axons and decreased myelin, although MRI overestimates the degree of demyelination with many regions of FLAIR abnormality being due to increased fluid rather than demyelination ¹⁷.

The pathophysiology of white matter lesions is different depending on the area of involvement, i.e. periventricular or deep (subcortical) white matter. This difference is emphasized in the Fazekas scale in which the two are separated. Pathogenesis and especially its clinical significance are still incompletely understood ^3,5,17.

Periventricular white matter lesions

Periventricular white matter changes (3-13 mm from the ventricular surface) are thought to be haemodynamically determined rather than only related to small vessel disease ⁸. This region is a vascular border zone vascularized by non-collateralising ventriculofugal vessels arising from subependymal arteries. As such, it is prone to local and systemic decrease in cerebral blood flow. It is a predictor of watershed infarcts especially when located along the posterior horns and it is correlated with carotid artery stenosis ⁸.

It is worth noting that juxtaventricular white matter changes (<3 mm from the ventricular surface), such as ependymitis granularis, are not related to small vessel disease, but rather represent cerebrospinal fluid leak due to disruption of the ependyma ¹⁰.

Deep and subcortical white matter lesions

Deep white matter changes (>13 mm from the ventricular surface, >4 mm from the corticomedullary junction) are thought to be caused by lipohyalinosis (small vessel disease), i.e. incomplete arteriosclerosis ^8,9. They are a predictor of lacunar infarcts.

Radiographic features

White matter changes

Chronic small vessel disease consists of bilateral patchy or diffuse white matter changes often observed on imaging studies ^6,7. The Fazekas scale has been proposed to quantify white matter lesions related to leukoaraiosis. This is especially useful in the setting of dementia.

CT

non-enhancing white matter hypodensities

MRI

T1: hypointense or isointense, less conspicuous than on T2/FLAIR
T2/FLAIR: hyperintense
DWI: no diffusion restriction
T1 C+ (Gd): non-enhancing

Other changes

In addition to white matter changes, cerebral small vessel disease may have a number of other radiographic manifestations ¹⁷. Please see individual articles for detailed description of these radiographic features ¹⁷:

History and etymology

The term leukoaraiosis means white matter rarefaction and comes from the Greek (leuko = white and araios = rarefaction). It was first proposed by Vladimir Hachinski (fl. 2021) a Ukrainian-born Canadian neurologist. He also coined the term multi-infarct dementia and developed the Hachinski ischemic score ^6,13.

Differential diagnosis

The differential causes of small vessel disease are enumerated above in the Etiology section.

Quiz questions

References

1. Amar K, Bucks R, Lewis T, Scott M, Wilcock G. The Effect of White Matter Low Attenuation on Cognitive Performance in Dementia of the Alzheimer Type. Age Ageing. 1996;25(6):443-8. doi:10.1093/ageing/25.6.443 - Pubmed
2. Amar K, Lewis T, Wilcock G, Scott M, Bucks R. The Relationship Between White Matter Low Attenuation on Brain CT and Vascular Risk Factors: A Memory Clinic Study. Age Ageing. 1995;24(5):411-5. doi:10.1093/ageing/24.5.411 - Pubmed
3. Helenius J, Soinne L, Salonen O, Kaste M, Tatlisumak T. Leukoaraiosis, Ischemic Stroke, and Normal White Matter on Diffusion-Weighted MRI. Stroke. 2002;33(1):45-50. doi:10.1161/hs0102.101228 - Pubmed
4. Pantoni L & Garcia J. Pathogenesis of Leukoaraiosis: A Review. Stroke. 1997;28(3):652-9. doi:10.1161/01.str.28.3.652 - Pubmed
5. Geerlings M, Appelman A, Vincken K, Mali W, van der Graaf Y, van der Graaf Y. Association of White Matter Lesions and Lacunar Infarcts with Executive Functioning: The SMART-MR Study. Am J Epidemiol. 2009;170(9):1147-55. doi:10.1093/aje/kwp256 - Pubmed
6. Hachinski V, Potter P, Merskey H. Leuko-Araiosis: An Ancient Term for a New Problem. Can J Neurol Sci. 1986;13(4 Suppl):533-4. doi:10.1017/s0317167100037264 - Pubmed
7. Grueter B & Schulz U. Age-Related Cerebral White Matter Disease (Leukoaraiosis): A Review. Postgrad Med J. 2012;88(1036):79-87. doi:10.1136/postgradmedj-2011-130307 - Pubmed
8. Kim K, MacFall J, Payne M. Classification of White Matter Lesions on Magnetic Resonance Imaging in Elderly Persons. Biol Psychiatry. 2008;64(4):273-80. doi:10.1016/j.biopsych.2008.03.024 - Pubmed
9. Xiong Y & Mok V. Age-Related White Matter Changes. J Aging Res. 2011;2011:617927. doi:10.4061/2011/617927 - Pubmed
10. Fazekas F, Schmidt R, Scheltens P. Pathophysiologic Mechanisms in the Development of Age-Related White Matter Changes of the Brain. Dement Geriatr Cogn Disord. 1998;9 Suppl 1(Suppl. 1):2-5. doi:10.1159/000051182 - Pubmed
11. Prins N & Scheltens P. White Matter Hyperintensities, Cognitive Impairment and Dementia: An Update. Nat Rev Neurol. 2015;11(3):157-65. doi:10.1038/nrneurol.2015.10 - Pubmed
12. Lee S, Kim J, Lee K et al. The Leukoaraiosis is More Prevalent in the Large Artery Atherosclerosis Stroke Subtype Among Korean Patients with Ischemic Stroke. BMC Neurol. 2008;8(1):31. doi:10.1186/1471-2377-8-31 - Pubmed
13. Goodman A. Vladimir Hachinski: A Pioneer in the Field of Stroke. Lancet Neurol. 2009;8(1):34. doi:10.1016/S1474-4422(08)70285-0 - Pubmed
14. Rosenberg G, Wallin A, Wardlaw J et al. Consensus Statement for Diagnosis of Subcortical Small Vessel Disease. J Cereb Blood Flow Metab. 2016;36(1):6-25. doi:10.1038/jcbfm.2015.172 - Pubmed
15. Pantoni L. Cerebral Small Vessel Disease: From Pathogenesis and Clinical Characteristics to Therapeutic Challenges. Lancet Neurol. 2010;9(7):689-701. doi:10.1016/S1474-4422(10)70104-6 - Pubmed
16. Wardlaw J, Smith E, Biessels G et al. Neuroimaging Standards for Research into Small Vessel Disease and Its Contribution to Ageing and Neurodegeneration. Lancet Neurol. 2013;12(8):822-38. doi:10.1016/S1474-4422(13)70124-8 - Pubmed
17. Haller S, Kövari E, Herrmann F et al. Do Brain T2/FLAIR White Matter Hyperintensities Correspond to Myelin Loss in Normal Aging? A Radiologic-Neuropathologic Correlation Study. Acta Neuropathol Commun. 2013;1(1):14. doi:10.1186/2051-5960-1-14 - Pubmed

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