Chronic cerebrospinal venous insufficiency is not associated with cognitive impairment in multiple sclerosis

Multiple sclerosis (MS) is an inflammatory disease of the central nervous system, causing both demyelination and neurodegeneration [1, 2]. As would be expected, a substantial number, roughly 50% [3‐5], of MS patients have cognitive impairment. In recently diagnosed or benign course patients, the incidence ranges from 20% to 40% [5, 6] whereas in samples with a substantial secondary progressive course, roughly 60% of patients are affected [4]. The correlation between cognitive impairment and brain atrophy is robust [7‐9]. However, why some patients show cognitive impairment and brain atrophy while others do not is poorly understood.

Chronic cerebrospinal venous insufficiency (CCSVI) was first reported in MS patients in 2009 [10]. As a vascular condition, CCSVI is characterized by anomalies of the main extra-cranial cerebrospinal venous routes, mainly in internal jugular and azygos veins that are hypothesized to interfere with normal venous outflow from the brain to the periphery. Since then, the topic has met with unprecedented controversy following a wide range of reported CCSVI frequencies in MS studies [11‐13]. Diagnosis of CCSVI implies a pathological condition the determination of which is based mainly on color Doppler sonography (DS) of extra- (neck) and intra-cranial veins using five venous hemodynamic (VH) criteria (with cutoff of ≥2 positive criteria used for a diagnosis of CCSVI) [10, 14]. So far, published studies comparing the prevalence of CCSVI in MS patients and controls [12, 15] have not reproduced the original findings of Zamboni et al. showing 100% sensitivity/specificity [10, 14]. While some groups did report a higher prevalence in MS patients than controls [16, 17], others reported the opposite, that is, no greater frequency in MS than in healthy persons [16, 18‐22]. In the largest cohort studied to date, we found a CCSVI frequency of 56.1% in MS patients compared to 22.7% in healthy controls [23]; however, the condition was also detected at a high frequency in patients with other neurologic diseases.

While not causative, some studies suggest that CCSVI may be a risk factor for clinical worsening in MS [24‐26], although here, too, there are contradictory results [16, 20]. In a large cohort study exploring the association between CCSVI status and both lesion burden and brain atrophy in MS, no relationship was found [27].

If CCSVI is a risk factor for neurodegeneration or progressive neurologic disability, we would expect significant correlation between CCSVI and cognitive impairment within MS cohorts. The present study was intended to examine this hypothesis.

Of the 109 patients enrolled, 79 were diagnosed with relapsing-remitting, 23 with secondary-progressive, and 7 with primary-progressive disease subtype. All were Caucasian, except two African-Americans and two of Latin American heritage. The other descriptive statistics including demographic, clinical, depression and cognitive outcomes are presented in Table 1. The CCSVI positive and negative MS groups were well matched, and no age, disease duration, EDSS or disease subtype differences were found. While the pattern of cognitive impairment was the same as described in previous studies (SDMT and BVMTR most sensitive), overall we found less impairment in this sample as compared to some previous studies using the same test battery [7, 45‐47].

There were 64 (58.7%) patients considered CCSVI-positive and 45 negative (Table 1). As shown in Figure 1, the total criteria VHISS score ranged 0 to 8. The median was represented by 26 patients achieving a score of 3.

The regression models predicting VHISS score after controlling for education and gender were not statistically significant for any of the MACFIMS predictor variables. The largest partial r in the analysis was −0.13 between CVLTR Delayed Recall and the VHISS score (Table 2).

The analysis of covariance (ANCOVA) tests showed a significant effect of CCSVI-positive diagnosis on cognitive ability in one of the 10 MACFIMS outcomes (Table 1, Figure 2). For BVMTR Delayed Recall, CCSVI-positive patients showed better performance than their CCSVI-negative counterparts (P = 0.009). The direction of the effect was thus counter to expectation in that positive patients achieved a score of 9.1 compared to 7.8 for the CCSVI negative group.

To the best of our knowledge, this is the first investigation of neuropsychological status in MS patients in relation to CCSVI. In this sample of 109 MS patients, we find no evidence of an association between CCSVI and cognitive impairment. Moreover, no relationship between cognitive performance and the severity of CCSVI criteria, as determined by DS, was detected in linear regression analysis. When patients were categorized by their CCSVI status (positive/negative), significant group differences emerged for only one test, in a direction contrary to the hypothesis that CCSVI is a risk factor for cognitive impairment in MS. Similarly, there was no relationship between CCSVI and depression in this cohort.

The CCSVI hypothesis has provoked great controversy and debate in the MS research community since it was first presented [11, 13]. The hypothesis gained popularity among MS patients because of the postulated possibility of venous insufficiency correction using endovascular procedures. While the diagnosis of CCSVI can be established using noninvasive and invasive imaging techniques [12], the validity of DS to establish the diagnosis of CCSVI remains controversial. We showed previously that DS, in properly trained hands, has high sensitivity and specificity for CCSVI diagnosis, when compared to invasive imaging methods [48, 49]. This was the same method as used in this study, and thus we are confident in the validity of the CCSVI categorization in our analysis.

The true prevalence of CCSVI in MS patients is unknown, and there is good evidence that the condition is also found in patients with other neurologic diseases [23]. In this study, 64% of the participating MS subjects presented with CCSVI, which is similar to our previous study [23]. The difference between the prevalence rates of CCSVI-positive versus -negative MS patients in this study is modest, and of uncertain meaning with respect to MS pathology. Indeed, emerging studies point against CCSVI having a primary causative role in the development of MS [11, 13]. A multimodal approach will likely be needed to determine the extent to which CCSVI is present in various healthy and disease groups and MS subtypes [15].

Cognitive impairment is common in MS and can be reliably quantified using neuropsychological tests emphasizing episodic memory, mental processing speed and some aspects of executive function [50]. Neuropsychological deficits are also robustly correlated with brain MRI measures, especially global and regional brain atrophy [51]. The heterogeneity of neuropsychological presentation among MS patients is influenced by many factors, including genetics, gender, intelligence, disease course, comorbid neuropsychiatric illness and health behaviors. The present study employed consensus standard tests emphasizing multiple domains of cognitive function, allowing us to test, in a comprehensive way, whether the presence and severity of CCSVI can influence this important sphere of disability in MS patients. No association between cognitive impairment and the presence and severity of CCSVI was found. This is consistent with our previous findings of a lack of association between the presence of CCSVI and severity of lesion burden and brain atrophy outcomes in MS patients [27].

There are a number of potential limitations in this study. Selection of participants was based on the inclusion or exclusion criteria in patients agreeing to undergo cognitive testing. However, it may be that the most severe patients presenting in our Center were not included in the study. Another potential limit is not including a control group. However, the aim of this study was not to assess CCSVI prevalence, but rather an association with cognitive impairment. Finally, the diagnosis of CCSVI was not confirmed by the use of other invasive diagnostic methods.

In conclusion, we find no evidence of an association between the presence and severity of CCSVI and cognitive impairment and depression in patients with MS.