Ward et al. reported the relationships between frailty index, healthy lifestyle and polygenic risk scores, and incident all-cause dementia (1). The adjusted hazard ratio (HR) (95% CI) of participants with high frailty for incident dementia was 3.68 (3.11 to 4.35). In addition, the adjusted HR (95% CI) of participants with high genetic risk and high frailty for incident dementia was 5.81 (4.01 to 8.42).The authors emphasized of controlling frailty for dementia prevention strategies, even among subjects at high genetic risk. I have two comments about their study.

First, Lourida et al. investigated the association between healthy lifestyles and risk of dementia by considering genetic risk (2). The adjusted HR (95% CI) of participants with high genetic risk and unfavorable lifestyle for incident dementia was 2.83 (2.09 to 3.83). In addition, a favorable lifestyle was associated with a lower dementia risk among participants with high genetic risk. There was no significant interaction between genetic risk and lifestyle factors, and I suppose that unfavorable lifestyles and genetic factors independently contribute to the risk of dementia. The level of frailty may be related to lifestyles and contribute to subsequent progression of cognitive impairment.

Second, Kojima et al. conducted a meta-analysis regarding the effect of frailty on the incident dementia among community-dwelling older people (3). Th pooled HRs (95% CIs) of frailty for the incident Alzheimer disease, vascular dementia, and all dementia were 1.28(1.00 to 1.63), 2.70 (1.40-5.23), and 1.33 (1.07 to 1.67), respectively. They also observed sex difference that frail women had a higher risk of incident Alzheimer disease than frail men. There is a report that the prevalence of Alzheimer disease in women is higher than that in men at the same generation (4), and frailty may also contribute to the risk of Alzheimer disease via sex-related factors.

References
1. Ward DD, Ranson JM, Wallace LMK, Llewellyn DJ, Rockwood K. Frailty, lifestyle, genetics and dementia risk. J Neurol Neurosurg Psychiatry 2021 Dec 21. doi: 10.1136/jnnp-2021-327396.
2. Lourida I, Hannon E, Littlejohns TJ, Langa KM, Hyppönen E, Kuzma E, Llewellyn DJ. Association of Lifestyle and Genetic Risk With Incidence of Dementia. JAMA 2019;322(5):430-437.
3. Kojima G, Taniguchi Y, Iliffe S, Walters K. Frailty as a Predictor of Alzheimer Disease, Vascular Dementia, and All Dementia Among Community-Dwelling Older People: A Systematic Review and Meta-Analysis. J Am Med Dir Assoc 2016;17(10):881-8.
4. Yoshida D, Ohara T, Hata J, Shibata M, Hirakawa Y, Honda T, Furuta Y, Oishi E, Sakata S, Kanba S, Kitazono T, Ninomiya T. Lifetime cumulative incidence of dementia in a community-dwelling elderly population in Japan. Neurology 2020;95(5):e508-e518.

There have been some studies investigating blood neurofilament light chain (NfL) levels as predictors of cognitive functions decline in neurological disorders. I want to discuss here the association between blood NfL levels and neuroaxonal damage in patients with brain damages including Alzheimer's disease and stroke by considering the underlying mechanisms.

First, Egle et al. reported that baseline increased serum NfL levels could predict cognitive decline and the risk of converting to dementia in a cerebral small vessel disease (SVD), but there was no change in serum NfL levels over a 5-year follow-up period [1]. The lack of dynamic changes of NfL in stroke stand in contrast to neurodegenerative disease, and serum NfL levels may not be used as a surrogate marker for monitoring cognitive impairment in patients with SVD. In contrast, Stokowskaet et al. examined plasma NfL levels for the prediction of functional improvement in the late phase after stroke [2]. The odds ratios (ORs) (95% confidence intervals [CIs]) of elevated plasma NfL levels for the improvement in balance and gait improvement were 2.34 (1.35-4.27) and 2.27 (1.25-4.32), respectively. In addition, OR (95% CI) of elevated plasma NfL levels for cognitive improvement was 7.54 (1.52-45.66), which was also verified by intervention trial. This study presented the usefulness of plasma NfL levels as a biomarker of physical and psychological function after stroke events. As there is a wide range of 95% CI of OR for cognitive improvement, unstable risk estimation may be updated by summing-up the events. Anyway, discrepancy in the results from two reports should be specified by further studies.

Second, Santangelo et al. examined predictors of cognitive decline rate to assess the risk of fast Alzheimer's disease (AD) progression [3]. Higher plasma NfL levels, worse scores at semantic verbal fluency and clock drawing test were significant predictors of fast progression in AD. Their regression model could predict 81.2% of patients' progression correctly, if all the three predictors were judged abnormal. Patients with AD present cognitive decline as a major neurological symptom and neuroaxonal damages are progressive. As conclusive results have been made whether blood NfL levels could substitute for information from neuroimaging and NfL levels in cerebrospinal fluids, further studies by using blood samples are needed to verify the association.

Regarding the second query, Lin et al. reported that high plasma NfL correlated with poor cognition in AD, and plasma NfL represented a biomarker of cognitive decline in AD [4]. Although the majority of studies found that blood NfL levels were inversely correlated with cognition, there are also positive relationships in some specific status of the neurological disorders, and individual differences and methodological procedures should be considered for the analysis [5]. Indeed, patients with AD have shown that intra-individual NfL changes were sensitive to detect the disease onset of neurodegenerative diseases [6].

In any case, the association between blood NfL levels and neuroaxonal damage in the brain during neurodegeneration may be mediated by disease-specific factors and fundamental biological factors such as sex and age.

References
1. J Neurol Neurosurg Psychiatry 2021;92(6):582-9.
2. Eur J Neurol 2021;28(7):2218-28.
3. Eur J Neurol 2021 Jun 27. doi: 10.1111/ene.14999
4. Sci Rep 2018;8(1):17368.
5. J Neurol Sci 2021;420:117229.
6. Nat Med 2019;25(2):277-83.

We recently published our preliminary case-control study showing that a medical history of hypothyroidism was more prevalent among COVID-19 patients with persistent olfactory dysfunction compared to controls (50% vs 8%; p=0.009) and that hypothyroidism was independently (p=0.021) associated with higher likelihood of persistent hyposmia/anosmia among patients with COVID-19 (OR: 21.1; 95%CI: 2.0 to 219.4) after adjusting for age and sex (1). As previously stated, our results are not -by any means- confirmatory of an etiologic association between hypothyroidism (or preferably chronic autoimmune thyroiditis, CAT, as aptly suggested by Rotondi et al.) and the development of persistent anosmia in COVID-19 patients (1). However, the suggetsed mechanism by Rotondi et al. strengthens our observations by proposing a possible biomolecular explanation behind our clinical observations. Indeed, chemokines that are induced by SARS-CoV-2 infection, and especially CXCL10, could act as effectors of demyelination of the central nervous system (CNS) - including the olfactory apparatus - through attraction and recruitment of T-lymphocytes (2,3). Although the proposed pathogenetic mechanism by Rotondi et al. needs further investigation and laboratory confirmation through experimental studies in COVID-19 patients with persistent olfactory dysfunction, it certainly invigorates our preliminary clinical results and sets the grounds for further research in a clinically significant post-COVID-9 sequela. Therefore, we are highly grateful to Rotondi and colleagues for their insightful and constructive comments in our study.

References
1. Tsivgoulis G, Fragkou PC, Karofylakis E, Paneta M, Papathanasiou K, Palaiodimou L, Psarros C, Papathanasiou M, Lachanis S, Sfikakis PP, Tsiodras S. Hypothyroidism is associated with prolonged COVID-19-induced anosmia: a case-control study. J Neurol Neurosurg Psychiatry. 2021.
2. Oliviero A, de Castro F, Coperchini F, Chiovato L, Rotondi M. COVID-19 Pulmonary and Olfactory Dysfunctions: Is the Chemokine CXCL10 the Common Denominator? Neuroscientist. 2020:1073858420939033.
3. Rotondi M, Chiovato L, Romagnani S, Serio M, Romagnani P. Role of chemokines in endocrine autoimmune diseases. Endocr Rev. 2007;28(5):492-520.

Dear Editor,
We have read with interest a recent paper by Seiffge and his colleagues published in your journal (1). In their study entitled as “Small vessel disease burden and intracerebral haemorrhage in patients taking oral anticoagulants”, the authors have investigated the role of small vessel disease on intracerebral hemorrhages (ICH) associated with the use of oral anticoagulation therapy. The authors showed that the small vessel disease with medium-to-high severity, detected by either computed tomography (CT) or magnetic resonance imaging (MRI), was significantly more prevalent in patients with ICH taking oral anticoagulants in compared to those without prior anticoagulation therapy (56.1% vs 43.5% on CT, and 78.7% vs 64.5% on MRI, respectively; p<0.001). Leukoaraiosis and atrophy were also reported to be more frequent and severe in patients with ICH related to anticoagulation therapy. We think that the results of the study are considerable emphasizing the importance of small vessel disease for ICH, which should therefore be implemented among the criteria of the risk stratification scores of bleeding.

The use of the scoring systems for the risk stratification of the intracranial bleeding is practically important in patients who are the candidates for the anticoagulation therapy. A recent study investigating the risk factors predicting ICH in patients with atrial fibrillation under anticoagulation therapy demonstrated that the presence of white matter changes was one of the risk factors being significantly higher in patients having ICH than controls (66.6% versus 32.5% respectively, p=0.0001) (2). On the other hand, the authors concluded that although the presence of white matter changes was one of the risk factors predicting ICH in patients with atrial fibrillation under anticoagulation therapy, it failed to show a significant association with CHA2DS2-VASc or HAS-BLED scores. While the use of validated scoring systems was encouraged in prediction of the ‘risk’ versus ‘benefit’ reasoning when deciding whether or not to start/resume oral anticoagulation therapy in patients with atrial fibrillation, this discrepancy tells us that these scoring systems may benefit from some revisions. Indeed, we have previously discussed the need for the revisions in HAS-BLED, and suggested the incorporation of the presence of white matter abnormalities and leukoaraiosis into the scoring system, in addition with the type of stroke (whether ischemic or hemorrhagic of type), and the localization of previous hemorrhages (whether deep versus lobar in location) (3,4). The latest guideline of the European Society of Cardiology (ESC) for the diagnosis and the management of atrial fibrillation have also emphasized that there is a prominent increase in the occurrence of ICH in parallel with the increase in the numbers of cerebral micro bleeds (5). On the other hand, the effects of cerebral micro bleeds on the treatment strategies were reported to be proven.

In the light of these data, it seems that some revisions are being required for the scoring systems, as supported by the recent study by Seiffge and his colleagues (1), demonstrating the importance of small vessel disease in patients with anticoagulation-associated ICH. The failure to demonstrate a significant association with the risk factors of ICH, including small vessel disease, and the CHA2DS2-VASc or HAS-BLED scores in the study by Paciaroni and his colleagues (2) may be explained, at least to some extent, by the shortcomings of the scoring systems to cover important risk factors of ICH in this group of patients, mainly the white matter abnormalities, leukoaraiosis, the type and the localization of previous strokes and the micro bleeds. In this era, the neuroimaging techniques are easily reachable in the detection of white matter abnormalities or cerebral micro bleeds, and the use of these data should be encouraged before a decision was made for the anticoagulation therapy. On these bases, we would like to emphasize the importance and the need for the revision in scoring systems to better cover the risk factors of ICH, which, we believe, will more adequately aid the (re)institution of the oral anticoagulation treatment.
References
1. Seiffge DJ, Wilson D, Ambler G, Banerjee G, Hostettler IC, Houlden H, et al. Small vessel disease burden and intracerebral haemorrhage in patients taking oral anticoagulants. J Neurol Neurosurg Psychiatry. 2021; jnnp-2020-325299.
2. Paciaroni M, Agnelli G, Giustozzi M, Caso V, Toso E, Angelini F, et al. Risk Factors for Intracerebral Hemorrhage in Patients With Atrial Fibrillation on Non-Vitamin K Antagonist Oral Anticoagulants for Stroke Prevention. Stroke. 2021;52(4):1450-1454.
3. Ince B, Benbir G, Gozubatik-Celik G. Should HAS-BLED scoring be revised for better risk estimation in patients with intracerebral hemorrhage? Expert Rev Cardiovasc Ther. 2014;12(8):929-931.
4. Ince B, Senel G. Deep versus lobar intracerebral hemorrhage on HAS-BLED scoring system. Chest. 2016;149(6):1589-1590.
5. Hindricks G, Potpara T, Dagres N, Arbelo E, Bax JJ, Blomström-Lundqvist C, et al; ESC Scientific Document Group. 2020 ESC Guidelines for the diagnosis and management of atrial fibrillation developed in collaboration with the European Association for Cardio-Thoracic Surgery (EACTS): The Task Force for the diagnosis and management of atrial fibrillation of the European Society of Cardiology (ESC) Developed with the special contribution of the European Heart Rhythm Association (EHRA) of the ESC. European Heart J. 2021;42(5):373–498.