Increased plasma neurofilament light chain levels in patients with type-1 diabetes with impaired awareness of hypoglycemia.

INTRODUCTION: Impaired awareness of hypoglycemia (IAH) is a common complication in patients with type-1 diabetes (T1D). IAH is a major risk factor for severe hypoglycemic events, leading to adverse clinical consequences and cerebral damage. Non-invasive, cost-effective, and logistically efficient biomarkers for this condition have not been validated. Here, we propose plasma neurofilament light chain (NfL) levels as a biomarker of neuroaxonal damage in patients with T1D-IAH. RESEARCH DESIGN AND METHODS: 54 patients were included into the study (18 T1D-IAH, 18 T1D with normal awareness of hypoglycemia (NAH) and 18 healthy controls). We measured plasma NfL levels and studied cerebral gray matter alterations on MRI.
RESULTS: We found that NfL levels were increased in patients with T1D-IAH compared with patients with T1D-NAH and healthy controls. Importantly, increased NfL levels correlated with reduced cerebral gray matter volume and increased IAH severity in patients with T1D-IAH.
CONCLUSION: Overall, our findings identify plasma NfL levels as a potential biomarker of cerebral damage in this population, motivating further confirmatory studies with potential implications in clinical trials. © Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.

Patients with type 1 diabetes (T1D) with impaired awareness of hypoglycemia (IAH) are in higher risk of severe hypoglycemia (SH).

SH is associated with adverse clinical consequences and cerebral damage.

There is no validated biomarker for this subgroup of patients.

Plasma neurofilament light chain (NfL) levels were increased in patients with T1D-IAH compared to patients with T1D with normal awareness of hypoglycemia and healthy controls.

Increased NfL levels correlated with reduced cerebral gray matter volume and increased IAH severity in patients with T1D-IAH.

Plasma Nfl levels could be used as a non-invasive, cost-effective, and logistically efficient biomarker of neuroaxonal damage in patients with T1D-IAH.

Introduction

About one in five patients with type 1 diabetes (T1D) have impaired awareness of hypoglycemia (IAH).1 IAH represents a risk factor for severe and recurrent hypoglycemic events, which can lead to brain damage.2 3 As no effective treatment has been clearly established,4 biomarkers capable of detecting and quantifying cerebral damage in this population are needed for the design of novel preventive or therapeutic strategies.

On the one hand, cerebral atrophy or functional impairment can be assessed using neuroimaging techniques. In fact, a structural and functional brain compromise has been described in patients with T1D-IAH.5 However, neuroimaging techniques have important limitations in terms of specificity, logistics, standardization, scalability, and cost-efficiency. On the other hand, while cerebrospinal fluid biomarkers of cerebral damage overcome some of these limitations, they require an invasive lumbar puncture procedure.

In recent years, research has focused on the detection of blood biomarkers of neural damage. Clearly, cost-efficient blood biomarkers would represent an accessible and centralizable alternative. However, the main challenge for the development of an adequate technology in this context has been the low blood concentration of proteins derived from the central nervous system (CNS). Importantly, in the last few years, the Single Molecule Array (Simoa) technology has shown unprecedented precision and sensitivity (ie, femtomolar range) for the quantification of blood biomarkers of brain damage.6 In particular, increased levels of neurofilament light chain (NfL) in blood have shown a great potential for the detection of neurodegeneration (neuronal loss and axonal damage), traumatic brain injury, and cerebrovascular accidents.7

In this brief report, we investigate whether patients with T1D with hypoglycemia unawareness show increased levels of plasma NfL compared with patients with normal awareness of hypoglycemia (NAH) and healthy controls (HC). Additionally, we explore whether abnormally increased NfL levels in this population correlate with IAH severity and reduced cerebral gray matter volume (GMV).

Materials and methods

Sample and assessments

A total of 54 participants were included in this study: 36 patients with T1D and 18 HC. Eighteen patients with T1D fulfilled clinical criteria for IAH (T1D-IAH) and the other 18 patients had NAH (T1D-NAH). Both T1D groups were selected as to have similar sociodemographics and T1D duration. The Clarke score was used for the IAH classification, which is based on eight questions that allow the determination of the glycemic threshold in which the patients notice the hypoglycemic symptoms.8 A Clarke score ≥4 was used to identify patients with T1D-IAH, whereas patients with T1D-NAH showed a score <3. The Clarke method comprises the following set of questions designed to characterize the participant’s exposure to hypoglycemia: Do you feel hypoglycemia symptoms when your blood glucose is low?, Have you lost symptoms of hypoglycemia that used to occur when your blood glucose is low?, Check all your symptoms of hypoglycemia over the last 6 months, If your answered ‘yes’ to any of the above question, how often do you have it?, Check all your symptoms of hypoglycemia over the last 12 months. If your answered ‘yes’ to any of the above question, how often do you have it? How often did you have an episode of hypoglycemia with symptoms during the last month? How often did you have an episode of hypoglycemia without symptoms during the last month? What was the lowest blood glucose level before feeling the symptoms of hypoglycemia? How often did you have symptoms of hypoglycemia when your blood glucose level was low?

The following exclusion criteria were applied: previous clinical diagnosis of cognitive impairment or neurological disorders, use of medications affecting the CNS, and MRI contraindications or intolerance. None of the participants in this study had any previous medical condition (apart from T1D) known to significantly alter blood NfL levels or cerebral GMV.

Both T1D groups were under similar insulin treatment, either as basal-bolus regimen or continuous subcutaneous insulin infusion (with short-acting insulin analogs). Sociodemographic, clinical, and laboratory data (diabetes and cardiovascular indicators) were recorded for each patient. Quantification of IAH severity was assessed, on one hand, by Clarke scores. On the other hand, we also recorded the number of severe hypoglycemic episodes during the last 5 years and the number of moderate hypoglycemic events during the last month. A severe hypoglycemic episode associated loss of consciousness, confusion/disorientation, seizures, or coma and required the assistance of a third person. A moderate hypoglycemic event was defined as any non-severe episode requiring the use of measures with impact on the daily life (interrupting work routine, stopping the car while driving, and so on). We combined both indicators to obtain a single indicator of the number of severe or moderate hypoglycemic episodes, providing a representative indicator of the clinical consequences of IAH.

Plasma NfL procedure

Blood was collected in EDTA tubes, centrifuged at 2000 g for 10 min and the plasma aliquoted in polypropylene tubes, and frozen at −80°C according to international consensus recommendations until analysis. Plasma NfL levels were measured with the Simoa Human NF-light Advantage kit using the Single Molecule Array technology (Simoa; Quanterix)9 in a SR-X Biomarker detection system by following the manufacturer’s instructions.

Neuroimaging acquisition and preprocessing

T1-weighted MRI scans were acquired in a Philips 3-Tesla station using a magnetization-prepared rapid acquisition with gradient echo protocol using the following parameters: flip angle 8°, repetition time 6.7 s, echo time 3.19 ms, pixel bandwidth 241, slice thickness 1.2 mm, and an acquisition matrix of size 256×256. All patients had available T1-MRI imaging, but nine subjects from the HC group did not have MRI data.

GMVs of the frontal, temporal, parietal, and occipital lobes for each participant were computed using the FreeSurfer 6.0 software package. Details about the standard FreeSurfer segmentation pipeline are available elsewhere (https://surfer.nmr.mgh.harvard.edu/). All preprocessed images were visually inspected to confirm the absence of segmentation errors.

Statistical analyses

Clinical, sociodemographics, NfL levels, and imaging data were compared across groups using one-way ANOVA (except χ2 for sex differences). Pairwise group differences were examined by general linear models including age, sex, education, and T1D duration as covariates of no interest. A logistic regression was also performed. In addition, we explored whether increased plasma NfL levels correlated with increased IAH severity or reduced GMV in patients with T1D. For that, we used one-sided Pearson’s correlation coefficients using the same nuisance covariates, for which a p<0.05 was considered significant.

Results

Table 1 shows the sample characteristics of this study. All groups had similar sociodemographics. There were no significant differences between T1D groups in terms of disease duration, cognitive status, or cardiovascular risk factors. However, as expected, patients with T1D-IAH showed increased Clarke scores and number of severe or moderate hypoglycemic events in the last month, reflecting common clinical consequences of IAH.

Table 1

Clinical, demographic, biomarker, and imaging information across groups

	T1D-IAH	T1D-NAH	HC	Significance (p value)
n	18	18	18
Age (years)	55.5±13.5	57.4±8.1	54.7±13.7	0.79
Sex (% female)	61%	27%	44%	0.13
Education (years)	14.8±5.1	14.7±4.4	13.6±3.5	0.64
Plasma NfL (pg/mL)	18.22±11.7	13.27±6.7	8.15±4.6	0.002*
T1D duration	31.7±12.8	30.2±8.6	NA	0.66
HbA1c (%)	7.57±1.1	7.60±0.8	NA	0.93
Body mass index (kg/m2)	25.9±6.6	27.2±3.8	NA	0.49
Mean arterial pressure (mm Hg)	93.6±15.6	101.8±13.6	NA	0.10
LDL-cholesterol (mg/dL)	96.3±27.4	94.6±21.3	NA	0.84
HDL-cholesterol (mg/dL)	71.4±16.5	63.7±19.1	NA	0.21
Clarke score	4.7±0.9	1.0±0.7	NA	<0.001*
Number of severe or moderate hypoglycemic episodes	4.89±6.3	0.61±1.0	NA	0.007*
Minimental state examination	29.56±0.6	29.61±0.8	NA	0.81
Frontal lobe GMV (mm3×10–3)	138.6±9.9	150.3±13.5	165.0±17.6	<0.001*
Temporal lobe GMV (mm3×10–3)	93.0±7.2	102.3±9.7	100.8±9.6	0.007*
Parietal lobe GMV (mm3×10–3)	89.6±8.7	97.3±9.4	108.2±8.8	<0.001*
Occipital lobe GMV (mm3×10–3)	41.7±4.8	48.3±6.8	45.1±6.6	0.008*

Values are expressed as mean±SD or percentage.

*P<0.05 three-group ANOVA/χ2 or t-test between T1D groups.

ANOVA, analysis of variance; GMV, gray matter volumes; HC, healthy controls; HDL, high-density lipoprotein; IAH, impaired awareness of hypoglycemia; LDL, low-density lipoprotein; NA, not applicable or available; NAH, normal awareness of hypoglycemia; NfL, neurofilament light chain; T1D, type-1 diabetes.

Significant differences were found across groups in plasma NfL, progressively increasing from HC to T1D-NAH and T1D-IAH. Pairwise NfL differences between T1D-IAH and T1D-NAH were significant after controlling for age, sex, education, and disease duration (β=0.039, p=0.038). A logistic regression to classify patients with T1D-IAH versus T1-NAH including all factors listed in table 1 (except for Clarke scores and number of hypoglycemic episodes) yielded the following results. Significance was only achieved by NfL levels (p=0.038), but the following close-to-significance factors were also observed: frontal GMV (p=0.062), temporal GMV (p=0.059), age (p=0.066), sex (p=0.064), and body mass index (p=0.054). Similarly, progressively decreasing GMV was observed across groups and cerebral lobules, and pairwise differences between T1D-IAH and T1D-NAH remained significant after controlling for the same nuisance covariates.

Finally, the following exploratory associations between increased NfL levels in patients with T1D and IAH severity and reduced cerebral GMV were observed. Within the T1D-IAH group, increased NfL levels correlated with lower frontal GMV (r=−0.51, p=0.030) and increased number of severe or moderate hypoglycemic events (r=0.49, p=0.038). When considering all patients with T1D, NfL levels correlated with Clarke scores (r=0.34, p=0.029) and the number of severe or moderate hypoglycemic events (r=0.45, p=0.005). Finally, although non-significant, NfL levels showed a mild association with temporal and parietal GMV (r=−0.28, p=0.051 and r=−0.21, p=0.11, respectively).

Figure 1 displays NfL differences across groups and a subset of these associations, using in some cases log NfL values to better illustrate group differences or correlations, for which all statistical results remained significant.

Figure 1

(A) Plasma NfL differences across groups (*p<0.05, **p<0.005). Scatter plots illustrating a subset of significant associations between NfL levels and (B) Clarke scores in patients with T1D, (C) frontal lobe GMV within the T1D-IAH group, and (D) number of severe or moderate hypoglycemic episodes within the T1D-IAH group. GMV, gray matter volumes; HC, healthy controls; IAH, impaired awareness of hypoglycemia; NAH, normal awareness of hypoglycemia; NfL, neurofilament light chain; T1D, type-1 diabetes.

Discussion

Our results reinforce the presence of increased brain damage in patients with T1D-IAH. Plasma NfL levels were increased in this population and correlated with reduced cortical gray matter and IAH severity. Therefore, plasma NfL could be a promising cost-efficient biomarker of neural damage in patients with T1D-IAH.

Patients with T1D-IAH showed reduced cerebral GMV, especially in the frontal lobe. A frontal compromise has been previously described in this population, both in neuroimaging and cognitive studies.5 10 Importantly, in patients with T1D-IAH, increased NfL levels correlated with reduced frontal GMV. This association shows that increased NfL levels reflect cerebral damage in this population, reinforcing its role as a potential biomarker. Moreover, increased NfL levels were also associated with increased IAH severity, as measured by Clarke scores and also by the number of severe or moderate hypoglycemic events. This further emphasizes the clinical significance of increased NfL levels in this population, which probably reflect neural damage due to recurrent hypoglycemia.

The main strength of this study is the inclusion of patients with T1D-IAH and T1D-NAH with similar T1D duration and sociodemographic and cardiovascular profiles. This allowed studying the effect of IAH on NfL levels and cerebral GMV with high specificity. Limitations of this work include the use of a relatively low sample size, some missing data in the control group, and the exploratory character of the correlations between NfL levels and IAH severity and GMV within the T1D-IAH group.

To conclude, we found that plasma NfL levels are increased in patients with T1D-IAH, probably reflecting the presence of neuroaxonal damage with clinical consequences. Overall, our findings motivate further confirmatory studies on the potential role of this biomarker in this population, which could be used to predict IAH or monitor cerebral damage in clinical trials.