Functional connectivity patterns in parosmia

Different degrees of parosmia were defined based on the responses to the 3 questions described above [7]. Parosmia degree 0 (Par 0) is defined as the group suffering from olfactory loss and no parosmia like symptoms, essentially the control group. Degree 1 (Par 1) refers to patients experiencing any one of the symptoms as described in the questionnaire. Par 1 patients developed parosmia 37 ± 19 weeks post anosmia or hyposmia. Degree 2 (Par 2) refers to patients exhibiting 2 symptoms whereas degree 3 (Par 3) includes patients with all the 3 symptoms. Since the number of patients suffering from Par 3 was small, we joined the Par 3 group and the Par 2 group, and labelled it as Par 2–3. Par 2–3 patients developed parosmia 40 ± 21 weeks post anosmia or hyposmia (Table 1). We did not control for duration of hyposmia as olfactory sensitivity was not significantly different between the parosmia groups as seen using ANOVA (F (2, 141) = 1.23, p = 0.45).

All scans were carried out using a 3 T MRI scanner (type Numaris; Siemens, Erlangen, Germany). A resting state functional scan using single shot echo-planar imaging (GRAPPA accelerator factor) with a TR = 2060 ms, TE = 25 ms, slice thickness = 4 mm, with no slice gap was acquired. The resting state scan lasted 8 min 22 s (240 measurements). A high resolution T1 MPRAGE was also acquired with the following parameters; TR = 1600 ms, TE = 3.01 ms, slick thickness = 1 mm. All functional analysis was carried out using FSLv6.0.2.

Data were pre-processed using FEAT (fMRI expert analysis tool), a part of FSL using an automated script [26, 27]. Pre-processing includes skull stripping using brain extraction tool (BET), motion correction using MCFLIRT, slice timing correction as TR > 1 s[28], spatial smoothing (6 mm full-width half maximum) and structural registration using skull stripped image of each participant to (Montreal Neurological Institute) MNI 2 mm brain (non-linear registration) using (FMRIB linear image registration tool) FLIRT. Noise signals were identified individually and removed using ICA-AROMA toolbox [29]. ICA-AROMA incorporates probabilistic Independent Component Analysis (ICA) on the partly pre-processed single-subject fMRI data (following spatial smoothing and normalization but before high-pass filtering), identifies independent components (ICs) representing motion artifacts and removes them from the fMRI time-series using linear regression. Group-level ICA with multi-session temporal concatenation was used to delineate global functional resting-state networks. Masking of non-brain voxels, voxel-wise de-meaning of the data and normalization of the voxel-wise variance were applied to the input data. ICA maps were thresholded at 0.5. The number of components was optimized using Laplace approximation to the Bayesian evidence of the model order [30]. Results of the group-ICA correspond to statistically independent components, that is, estimates of functional resting state networks (RSNs). The set of spatial maps from the group-average analysis was used to generate subject-specific versions of the spatial maps, and associated timeseries, using “dual_regression” [31]. First, for each subject, the group-average set of spatial maps is regressed (as spatial regressors in a multiple regression) into the subject's 4D space–time dataset. This results in a set of subject-specific time series, one per group-level spatial map. Next, those time series are regressed (as temporal regressors, again in a multiple regression) into the same 4D dataset, resulting in a set of subject-specific spatial maps, one per group-level spatial map. We then tested for [group differences, etc.] using FSL's randomize permutation-testing tool using general linear model (GLM) which defined to create a multiple subject design matrix with three groups.

To further explore whether there is altered FC even at the level of individual brain structures, we employed time series-based analysis in the ROIs, bilateral piriform cortex (PC) and orbitofrontal cortex (OFC). The ROIs are validated and can be found in already published studies [32]. The first step includes applying appropriate transforms to the ROIs since they are defined in structural space. Hence, they cannot be used for functional analysis. This is done using fslutilites, “applywarp”. The next step is to extract the time series from the warped ROI, which is performed by “fslmeants” command. Once the time series is extracted, single subject analysis is carried out which is similar to fMRI analysis [27], followed by group level analysis for each ROI [20].

All statistical analysis, unless stated otherwise, was carried using statistical software GraphPad Prism version 8.0. Whole brain ICA results using dual regression are by default reported at pFWE < 0.05. ROI based results are reported using Z statistic images which were thresholded non-parametrically using clusters determined by Z > 3.1 and a (corrected) cluster significance threshold of p < 0.05 [33].

A one-way ANOVA showed no age-based differences between groups (F (2, 141) = 0.13, p = 0.88). In addition, post-hoc multiple comparisons (Tukey) revealed no significant differences among groups. A non-significant chi-square test showed no differences in gender distribution among the groups [X² (1.75, 2 = 0.41)]. Also, no significant differences were found for olfactory threshold scores among the groups using ANOVA with multiple comparisons [F (2, 141) = 1.16, p = 0.31]. The demographics can be seen in Table 1.

A total of ten components (Fig. 2) were identified as RSNs from a group ICA analysis which included, visual network, default mode network (DMN), executive control network, sensorimotor network, medial visual network, left and right fronto-parietal network, visuo-spatial network, dorsal attentional network [34] and salience network [35]. The regions in the Salience network and Executive control network, in which Par 1 group showed significantly lower temporal concatenation (coherence) as compared to Par 0 group, include regions surrounding caudate nucleus and putamen and supramarginal gyrus (Fig. 3, top). Similarly, regions in the Medial visual network, in which Par 2–3 group showed significantly lower temporal concatenation as compared to both Par 0 and Par 1 group include bilateral thalamus and subcallosal cortex (Fig. 3, bottom). For other contrasts, brain activations did not survive multiple comparisons.

Piriform cortex (PC) and orbitofrontal cortex (OFC) were the regions chosen to carry out ROI-based FC chosen to understand the effect of parosmia on primary and secondary olfactory areas. Comparing groups, for seed right OFC: temporal pole and supramarginal gyrus were found to be significant and more functionally connected in Par 1 as compared to Par 2–3 (Fig. 4). Similarly, for the right PC, dorso-lateral pre-frontal cortex (dlPFC) was significantly more connected in Par 0 as compared to Par 2–3 (Fig. 4). For other contrasts, brain activations did not survive multiple comparisons.

Absence of an objective and standardized assessment tool for parosmia poses a significant challenge. As one has to rely on self-reported altered olfactory perceptions, it introduces subjectivity and lack of uniformity in evaluation. Another limitation of the study is the failure to include a depression measuring questionnaire for factoring in affects leading to changes in resting state FC.