Introduction:

Obsessive-compulsive disorder (OCD) is a neuropsychiatric disease characterized by distressing thoughts or urges that often require repetitive behaviors to suppress. OCD affects 2-3% of the general population and can have debilitating effects on normal functioning.[1] While most cases of OCD can be addressed through psychotherapy and/or medication, about 10% remain refractory, requiring neurosurgical intervention, such as neuroablation (ABL) or deep brain stimulation (DBS). These options possess their own respective advantages and disadvantages. ABL lacks the hardware concerns of DBS (e.g. device failure, battery replacement, etc.) and may be incisionless (e.g. stereotactic radiosurgery). Alternatively, DBS is non-lesional, and stimulation parameters can be titrated. While both ABL and DBS appear to be effective for refractory OCD, there is no clear consensus on their relative superiority/non-inferiority.

Our group previously sought to address this question by comparing the two treatments’ relative utility. [1] Using a random-effects, inverse-variance weighted meta-analysis of 56 studies, utility was calculated from Yale-Brown Obsessive Compulsive Scale (Y-BOCS) scores and adverse event (AE) incidence. In our analysis, no significant differences were found between stereotactic radiosurgery and radiofrequency ablation, so their studies were combined and all considered under ABL. Ultimately, ABL yielded a significantly greater utility compared to DBS (0.189±0.03 vs. 0.167±0.04, respectively; P<0.001). Due to perceived advantages of DBS over ABL, this result was surprising and inquiries were raised about the reliability of the analysis. A primary concern was whether study rigor could have impacted our finding. In this follow-up study, we performed an in-depth assessment of rigor of the ABL vs. DBS studies that previously met criteria for inclusion.

Methods:

Assessment of rigor requires the selection of a grading scale. However, as rigor scales are designed for a specific type of study, a single type of scale is incapable of properly assessing the variety of analyzed study types (e.g., RCT, cohort, and case series). To circumvent this issue, we decided to score only case series because they were the most common study type in both treatment groups. These studies were assessed with the Institute of Health Economics (IHE) quality appraisal checklist, which is a validated scale designed exclusively for case series.[2,3] These rigor scores were then used as covariates to a mixed-effects model of treatment against outcome (i.e. Y-BOCS score, adverse event (AE) incidence, and overall utility).

Results:

There were a total of 20 DBS and 17 ABL case series used in the meta-analysis; they represent 71.4% and 94.4%, respectively, of all studies in each treatment group. For overall number of patients, case series contribute 68.7% (125/182) and 97.7% (347/355) to DBS and ABL groups, respectively. In addition, they represent 40% (4/10) and 83.3% (10/12) of DBS and ABL studies that report AE incidence. DBS studies had significantly higher rigor scores than ABL studies (13.5/20 versus 11.0/20, respectively; p<0.001).

Similar to the results of Kumar et al., ABL still imparts a significantly higher utility than DBS with rigor as covariate in the mixed-effects model of treatment (p<0.0001). AE incidence was also significantly lower in ABL case studies (p=0.0024). For Y-BOCS score, ABL case series report greater percent reduction compared to DBS studies, though it was only marginally significant (p=0.0609). When rigor added to the mixed-effects model of treatment against outcome, neither the treatment group nor the rigor scores were significant predictors of % Y-BOCS score reduction (p=0.2261 and 0.4179, respectively). Similarly, neither treatment group nor rigor was a significant predictor of AE incidence (p=0.2223 and 0.4602, respectively). When considered as the sole predictor, rigor was not found to be significant predictor of % Y-BOCS score reduction (p = 0.1115). However, higher rigor scores were predictive of higher AE incidence (p = 0.0064).

Discussion:

Rigor is an important consideration as it may lend insight to a study’s validity and robustness. One hypothesis of ABL’s superiority over DBS was that ABL studies were less rigorous, producing outcomes that may be less reflective of reality. As rigor was not a significant covariate for utility, it suggests that Kumar et al.’s original conclusion of ABL superiority is accurate. However, even though rigor is not a significant covariate of % Y-BOCS score reduction, it is a significant predictor for AE incidence. Higher rigor studies generally had a higher reported AE incidence.

A notable limitation to this analysis is the exclusive use of case series. The mixed collection of study types precluded the perfect fit of a single scale to all studies. Since case series only represent a portion of all studies, our calculations slightly vary from those reported previously in Kumar et al. Nevertheless, case series represent the vast majority of studies and patients in both DBS and ABL groups. Though not a perfect facsimile, they are still highly representative. Regarding AE incidence, DBS case series constitute only 40% of overall DBS studies with AE reports. Yet, they were sufficient in establishing the significant association of high rigor and AE incidence. Given that the remaining DBS studies likely have even higher rigor (i.e. RCTs and cohort studies), an even stronger association with their inclusion is not an unreasonable inference. Furthermore, although treatment types were no longer significant predictors, this may be a consequence of working with fewer studies and overfitting data.

While study rigor was not a significant covariate for the current utility calculation, it is nevertheless an important consideration for similar meta-analyses, especially when assessing older and newer technologies. As the field of functional neurosurgery advances, there will be a greater need for similar comparisons to evaluate and guide clinical decision-making and adoption of novel techniques. Developments in DBS technologies can all plausibly improve DBS utility for OCD, necessitating further studies. Despite its limitations as an imperfect measure, study rigor may provide valuable insight into the reliability of reported data.

Bibliography:

1. Kumar KK, Appelboom G, Lamsam L, et al. Comparative effectiveness of neuroablation and deep brain stimulation for treatment-resistant obsessive-compulsive disorder: A meta-analytic study. J Neurol Neurosurg Psychiatry 2019;90:469–73. doi:10.1136/jnnp-2018-319318
2. Institute of Health Economics. Quality Appraisal Checklist for Case Series Studies. 2014;:1–2.
3. Guo B, Moga C, Harstall C, et al. A principal component analysis is conducted for a case series quality appraisal checklist. J Clin Epidemiol 2016;69:199–207.e2. doi:10.1016/j.jclinepi.2015.07.010

Verde et al. conducted a prospective study to determine the diagnostic and prognostic performance of serum neurofilament light chain (NFL) in patients with amyotrophic lateral sclerosis (ALS) (1). Serum NFL positively correlated with disease progression rate in patients with ALS, and higher levels were significantly associated with shorter survival. In addition, serum NFL did not differ among patients in different ALS pathological stages, and NFL levels were stable over time within each patient. I have a concern about their study.

Gille et al. also recognized the relationship of serum NFL with motor neuron degeneration in patients with ALS (2). They also recognized that serum NFL was significantly associated with disease progression rate and survival. Serum NFL can be recommended as a surrogate biomarker of ALS.

Regarding the first concern, Thouvenot et al. also checked if serum NFL can be used as a prognostic marker for ALS at the time of diagnosis (3). By Cox regression analysis, NFL, weight loss and site at onset were independent predictive factors of mortality, and higher NFL concentration at the time of diagnosis is the strongest prognostic fact

I recently discussed on serum neurofilament light chain in patients with amyotrophic lateral sclerosis (4), and these consistent results should also be verified by a meta-analysis of prospective studies.

References

1. Verde F, Steinacker P, Weishaupt JH, et al. Neurofilament light chain in serum for the diagnosis of amyotrophic lateral sclerosis. J Neurol Neurosurg Psychiatry. 2019 Feb;90(2):157-164. doi: 10.1136/jnnp-2018-318704

2. Gille B, De Schaepdryver M, Goossens J, et al. Serum neurofilament light chain levels as a marker of upper motor neuron degeneration in patients with amyotrophic lateral sclerosis. Neuropathol Appl Neurobiol. 2019;45(3):291-304. doi: 10.1111/nan.12511

3. Thouvenot E, Demattei C, Lehmann S, et al. Serum neurofilament light chain at time of diagnosis is an independent prognostic factor of survival in amyotrophic lateral sclerosis. Eur J Neurol. 2020;27(2):251-257. doi: 10.1111/ene.14063

4. Kawada T. Serum neurofilament light chain in patients with amyotrophic lateral sclerosis. Eur J Neurol. 2020 Mar 18. doi: 10.1111/ene.14223

Kaji et al. evaluated the efficacy and safety of intramuscular ultra-high-dose methylcobalamin in 373 patients with amyotrophic lateral sclerosis (ALS) (1). The primary endpoints were death or full ventilation support. Although there was no significant difference between treated and control group, 50 mg methylcobalamin-treated patients with early start within 12 months' duration of diagnosis showed longer time intervals to the primary event and keep the Revised ALS Functional Rating Scale (ALSFRS-R) score than the placebo group. The adverse effects by this treatment were similar and low prevalence among placebo, 25 mg or 50 mg groups. The authors recommend to verify the prognosis by this medication, and I have some concerns about their study.

First, the authors did not allow the change of riluzole administration and did not handle patients with edaravone treatment. I think that the vitamin B12 analog treatment in combination with recent neuro-protective drugs might be acceptable for future trials (2). In addition, the efficacy for ALS by methylcobalamin should be specified by adjusting several confounders for the analysis.

Relating to vitamin therapy for ALS, Rosenbohm et al. investigated the association of serum retinol-binding protein 4 (RBP4) with the onset and prognosis of ALS (3). Adjusted ORs (95% C) of the highest quartile of RBP4 against lowest quartile for incident ALS was 0.36 (0.22-0.59). In addition, serum RBP4 was inversely associated with mortality by survival analysis. RBC4 can be considered as a biomarker for insulin resistance and vitamin A metabolism, and the lack of vitamin A and insulin resistance might also be related to the pathogenesis of ALS.

Finally, other medications for ALS treatment can be considered for the analysis. Freedman et al. examined the association between lipid-lowering medication and ALS risk (4). Adjusted odds ratios (ORs) (95% confidence interval [CI]) of statins and fibrates for ALS were 0.87 (0.83-0.91) and 0.88 (0.80-0.97), respectively. In contrast, other three cholesterol-lowering medications such as nitrates, bile acid sequestrants and ezetimibe did not significantly associate with ALS. Although confounders and mediators cannot be clearly identified for the prognosis of ALS, basic parameters such as smoking and body mass index might be important variables for the adjustment.

REFERENCES

1 Kaji R, Imai T, Iwasaki Y, et al. Ultra-high-dose methylcobalamin in amyotrophic lateral sclerosis: a long-term phase II/III randomised controlled study. J Neurol Neurosurg Psychiatry 2019;90:451-7.

2 Ito S, Izumi Y, Niidome T, et al. Methylcobalamin prevents mutant superoxide dismutase-1-induced motor neuron death in vitro. Neuroreport 2017;28:101-7.

3 Rosenbohm A, Nagel G, Peter RS, et al. Association of serum retinol-binding protein 4 concentration with risk for and prognosis of amyotrophic lateral sclerosis. JAMA Neurol 2018;75:600-7.

4 Freedman DM, Kuncl RW, Cahoon EK, et al. Relationship of statins and other cholesterol-lowering medications and risk of amyotrophic lateral sclerosis in the US elderly. Amyotroph Lateral Scler Frontotemporal Degener 2018;19(7-8):538-46.

Dear Editor,
The original article by Jeppsson et al. provides substantial perspectives regarding the diagnostic
significance of cerebrospinal fluid (CSF) biomarkers in discriminating patients with idiopathic normal pressure hydrocephalus (iNPH) from patients with other neurodegenerative disorders. 1 They have found that patients with iNPH had, compared with healthy individuals, lower concentrations of P-tau and APP-derived proteins in combination with elevated MCP-1 1. Moreover, compared with the non-iNPH disorders group, iNPH was characterized by the same significant change; low concentration of tau proteins and APP-derived proteins, and elevated MCP-1. I sincerely appreciate the authors for conducting such a large-scale study of a strictly interesting topic. However, I would like to make some comments hoping to provide a better understanding of some points and some perspectives to be kept in mind while planning future related studies
In my opinion, the investigation of CSF biomarkers in patients with iNPH may provide several insights in addition to discriminating the iNPH patients from other neurodegenerative diseases. Certainly, these study results may give the opportunity to understand the unknown pathophysiological aspects of iNPH, thereby, even leading to new classifications of the disease. Actually, there may be many questions to be clarified regarding diagnostic approach, evaluation of the iNPH patients and even identification of the disease. 2,3 For instance, the diagnosis of iNPH may be a considerably challenging issue knowing that the full triad of NPH is present in under 60% of patients and the individual components of this triad are nonspecific as they may be encountered in many other neurodegenerative disorders. 2 Nevertheless, the gold standard of the diagnosis has been indicated as the short-term response to CSF drainage. 3,4 On the other hand, although a substantial rate of patients with iNPH improve by shunt surgery (80%), a crucial topic of discussion may be that why some subgroup of patients do not benefit from shunt surgery? Some authors have suggested that the presence of a possible underdiagnosed neurodegenerative disease might the main cause of shunt unresponsiveness in this patient subgroup. Arrestingly, in patients with iNPH, the high rates of the neurodegenerative comorbidities have been reported, several times. 3,5 Besides, it is acknowledged that although the presence of comorbidities does not exclude the possibility of iNPH; comorbidities do influence the prognosis after shunt surgery. 5 More interestingly, Espay et al. preferred to identify some subgroup of patients as the hydrocephalic presentations of neurodegenerative disorders (rather than NPH). 3 However, I believe that many of these discussions may be elucidated in the era of CSF biochemical investigations. Considering the various unknown aspects about the pathophysiology and pathogenesis of iNPH, the sufficiency of the current diagnostic criteria basing on the clinical triad, neuroimaging and short-term response to CSF diversion may also be interrogated. Based on the rationale of that treatment response is a critical clue providing insights about the underlying pathophysiology, I think that the response to shunt surgery may potentially be a crucial criteria to be kept in mind while diagnosing and classifying the patients with the current diagnosis of iNPH. 6 Hence, the use of CSF biomarkers may give promising conclusions for a better understanding of the iNPH pathophysiology and provide possible new classification criteria of the disease. Besides, it is remarkable to state that iNPH has been basically explained via mechanisms of CSF dynamic disturbance, mechanical stretching of periventricular tissue by the enlarging ventricles, impairment of blood-brain barrier, impaired periventricular blood flow associated to interstitial edema, ependyma disruption, microvascular infarctions, gliosis. However, there is no notable clue to classify iNPH as a primary neurodegenerative disease. On the other hand, secondary mechanisms including disturbed elimination of neurotoxic substances such as β-amyloid, tau-protein, and pro-inflammatory cytokines (basically associated with disturbed CSF turnover) have been hypothesized to be involved in the deterioration of iNPH clinic. 7,8 Ergo, investigations of CFS biomarkers in patients with iNPH may also give substantial perspectives regarding the pathophysiological features of iNPH which might be significantly varying among iNPH patients according to the current diagnostic criteria. 6 Furthermore, although it was not investigated in this study, 1 I think that analyzing the differentiating features of CSF biomarkers in iNPH patients benefiting and non-benefiting by shunt surgery would give substantial perspectives about the discussions mentioned above. The authors refer to the previous two reports 9,10 and indicate that there have not been any promising investigations on the use of CSF biomarkers to separate responders from non-responders. Nevertheless, I would like to remind that the mentioned reports included a limited number of patients and, actually, in the report by Miyajima et al., sAPPa was found as a suitable biomarker for also the prognosis of iNPH. 9 Therefore, in my opinion, the investigation of the significance of CSF biochemical pattern in distinguishing the NPH patients of shunt responders and non-responders, certainly constitutes a crucial topic of interest. The CSF biochemical patterns may also be investigated in patients with the current diagnosis of secondary NPH which have been acknowledged to have higher treatment (shunt) response rates in comparison to patients with iNPH. 11,12 In addition, the results of these mentioned studies may provide clues about the critical question of that what extent of the reversibility of the disease is due to the mechanical factors or a possible recovery of an underlying neurodegenerative process, thereby providing crucial insights about the primary underlying pathophysiology.
Abbreviations: CSF; Cerebrospinal fluid, APP; amyloid precursor protein, MCP-1; monocyte chemoattractant protein 1
Acknowledgments: None.
Funding: None.
Conflict of interests: None.

References
1. Jeppsson A, Wikkelso C, Blennow K, et al. CSF biomarkers distinguish idiopathic normal pressure hydrocephalus from its mimics. J Neurol Neurosurg Psychiatry. Jun 5 2019.
2. Marmarou A, Young HF, Aygok GA, et al. Diagnosis and management of idiopathic normal-pressure hydrocephalus: a prospective study in 151 patients. J Neurosurg. Jun 2005;102(6):987-997.
3. Espay AJ, Da Prat GA, Dwivedi AK, et al. Deconstructing normal pressure hydrocephalus: Ventriculomegaly as early sign of neurodegeneration. Ann Neurol. Oct 2017;82(4):503-513.
4. Ishikawa M, Guideline Committe for Idiopathic Normal Pressure Hydrocephalus JSoNPH. Clinical guidelines for idiopathic normal pressure hydrocephalus. Neurol Med Chir (Tokyo). Apr 2004;44(4):222-223.
5. Williams MA, Malm J. Diagnosis and Treatment of Idiopathic Normal Pressure Hydrocephalus. Continuum (Minneap Minn). Apr 2016;22(2 Dementia):579-599.
6. Relkin N, Marmarou A, Klinge P, Bergsneider M, Black PM. Diagnosing idiopathic normal-pressure hydrocephalus. Neurosurgery. Sep 2005;57(3 Suppl):S4-16; discussion ii-v.
7. Kudo T, Mima T, Hashimoto R, et al. Tau protein is a potential biological marker for normal pressure hydrocephalus. Psychiatry Clin Neurosci. Apr 2000;54(2):199-202.
8. Kondziella D, Sonnewald U, Tullberg M, Wikkelso C. Brain metabolism in adult chronic hydrocephalus. J Neurochem. Aug 2008;106(4):1515-1524.
9. Miyajima M, Nakajima M, Ogino I, Miyata H, Motoi Y, Arai H. Soluble amyloid precursor protein alpha in the cerebrospinal fluid as a diagnostic and prognostic biomarker for idiopathic normal pressure hydrocephalus. Eur J Neurol. Feb 2013;20(2):236-242.
10. Jeppsson A, Holtta M, Zetterberg H, Blennow K, Wikkelso C, Tullberg M. Amyloid mis-metabolism in idiopathic normal pressure hydrocephalus. Fluids Barriers CNS. Jul 29 2016;13(1):13.
11. Borgesen SE. Conductance to outflow of CSF in normal pressure hydrocephalus. Acta Neurochir (Wien). 1984;71(1-2):1-45.
12. Daou B, Klinge P, Tjoumakaris S, Rosenwasser RH, Jabbour P. Revisiting secondary normal pressure hydrocephalus: does it exist? A review. Neurosurg Focus. Sep 2016;41(3):E6.