| Literature DB >> 26565967 |
Fahmy Aboulenein-Djamshidian1,2, Martin Krššák3,4, Nermin Serbecic5,6, Helmut Rauschka1,2, Sven Beutelspacher6, Ivica Just Kukurová3, Ladislav Valkovič3, Adnan Khan7, Daniela Prayer8, Wolfgang Kristoferitsch2.
Abstract
BACKGROUND: To date, no direct scientific evidence has been found linking tissue changes in multiple sclerosis (MS) patients, such as demyelination, axonal destruction or gliosis, with either steady progression and/or stepwise accumulation of focal CNS lesions. Tissue changes such as reduction of the retinal nerve fiber layer (RNFL) and the total macular volume (TMV), or brain- and spinal cord atrophy indicates an irreversible stage of tissue destruction. Whether these changes are found in all MS patients, and if there is a correlation with clinical disease state, remains controversial. The objective of our study was to determine, whether there was any correlation between the RNFL or TMV of patients with MS, and: (1) the lesion load along the visual pathways, (2) the ratios and absolute concentrations of metabolites in the normal-appearing white matter (NAWM), (3) standard brain atrophy indices, (4) disease activity or (5) disease duration.Entities:
Mesh:
Year: 2015 PMID: 26565967 PMCID: PMC4643899 DOI: 10.1371/journal.pone.0142272
Source DB: PubMed Journal: PLoS One ISSN: 1932-6203 Impact factor: 3.240
Clinical data.
| before OCT examination | in further follow-up | ||||||||
|---|---|---|---|---|---|---|---|---|---|
| MS | age at | therapy | relapses | ON | age at | therapy was changed to | |||
| No | subtype | sex | onset | right | left | OCT/ MRI-MRS | |||
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| RRMS | f | 34.5 | MITOX, GLAT, IFN(b), IFN(a) | 7 | 0 | 0 | 40.5 | natalizumab |
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| RRMS | f | 18.5 | IFN(a), IFN(b) | 4 | 0 | 0 | 23.5 | natalizumab |
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| RRMS | f | 36.0 | MITOX | 7 | 0 | 0 | 42.0 | natalizumab |
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| RRMS | f | 31.5 | none | 3 | 0 | 0 | 38.0 | none |
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| RRMS | m | 40.0 | IFN(a) | 3 | 0 | 0 | 45.5 | none |
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| RRMS | f | 28.5 | IFN(b) | 3 | 0 | 0 | 39.0 | natalizumab |
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| RRMS | f | 43.0 | GLAT, IFN(b), none | 4 | 0 | 0 | 48.0 | natalizumab |
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| RRMS | f | 40.0 | none | 2 | 0 | 0 | 42.25 | none |
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| RRMS | m | 24.0 | none | 2 | 0 | 0 | 25.0 | none |
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| RRMS | f | 18.0 | GLAT, none | 2 | 0 | 0 | 19.75 | none |
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| RRMS | f | 29.75 | IFN(a) | 4 | 0 | 0 | 36.0 | none |
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| RRMS | m | 31.0 | IFN(b) | 2 | 0 | 0 | 33.25 | IFN(b) |
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| RRMS | m | 51.0 | IFN(b) | 2 | 0 | 0 | 52.0 | IFN(b) |
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| RRMS | m | 27.5 | GLAT | 4 | 0 | 0 | 39.0 | GLAT |
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| RRMS | f | 30.0 | IFN(b) | 4 | 0 | 0 | 46.0 | none |
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| RRMS | m | 39.0 | IFN(c) | 4 | 0 | 0 | 45.0 | IFN(c) |
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| RRMS | f | 16.0 | GLAT | 4 | 0 | 0 | 61.0 | GLAT |
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| RRMS | f | 26.0 | IFN(a), IFN(b), MITOX | 9 | 1 | 1 | 32.0 | none |
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| RRMS | f | 17.75 | IFN(a), IFN(b) | 6 | 1 | 3 | 19.75 | natalizumab |
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| RRMS | f | 31.0 | IFN(a), IFN(b) | 4 | 1 | 0 | 36.0 | IFN(b) |
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| RRMS | f | 20.0 | IFN(b) | 8 | 1 | 1 | 47.5 | IFN(b) |
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| RRMS | m | 22.5 | GLAT, IFN(a), IFN(b), natalizumab | 10 | 0 | 1 | 42.5 | natalizumab |
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| RRMS | f | 20.0 | IFN(a) | 3 | 0 | 4 | 41.0 | IFN(a) |
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| SPMS | m | 40.0 | GLAT, MITOX | 3 | 0 | 0 | 46.5 | none |
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| SPMS | f | 13.0 | IFN(b), MITOX | 5 | 0 | 0 | 27.0 | none |
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| SPMS | m | 25.0 | IFN(c), GLAT, IFN(a), IFN(b) | 10 | 1 | 1 | 47.5 | IFN(b) |
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| SPMS | m | 22.0 | IFN(b) | 5 | 1 | 0 | 30.5 | none |
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| SPMS | f | 16.0 | IFN(a), MITOX | 6 | 0 | 2 | 44.25 | none |
ON, optic neuritis;
*, relapses treated with high dose steroid pulse therapy; no included patient had an ON within 12 months prior to the beginning of the study;
GLAT, glatiramer-acetate 20mg subcutaneous once daily; MITOX, mitoxantrone; IFN(a), interferon beta 1a intramuscularly once per week; IFN(b), interferon beta 1a (44μg) subcutaneous trice per week; IFN(c), interferon beta 1b (250μg) subcutaneous alternate day. Most importantly, the disease activity remained high in further follow-up with a median observation period of 22 ± 0.5 months [33]. However, no significant reduction of either the RNFL or the TMV could be found in follow-up [33; 36].
1, discontinued (48mg mitoxantrone per m2 body surface); none, neither specific immunomodulatory or immunsuppressive therapy, drug holiday;
2, drug withdrawal 12 months before OCT examination;
3, drug withdrawal 6 months before OCT examination;
4, drug withdrawal 20 months before OCT examination;
5, high titres of anti-interferon autoantibodies, drug withdrawal 14 months before OCT examination;
6, mitoxantrone cumulative dose 96mg per m2 body surface, drug withdrawal 10 months before OCT examination;
7, mitoxantrone cumulative dose 92mg per m2 body surface, drug withdrawal 10 months before OCT examination;
8, mitoxantrone cumulative dose 92mg per m2 body surface, drug withdrawal 26 months before OCT examination;
9, mitoxantrone cumulative dose 108mg per m2 body surface, drug withdrawal 27 months before 1st OCT examination.
RNFL in MS patients.
| Group | G | G | T | TS | TI | S | I | N | NS | NI | T | TS | TI | S | I | N | NS | NI |
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| OD | OS | OD | OD | OD | OD | OD | OS | OS | OS | OS | OS | OS | OS | OS | OD | OD | OD | |
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| STE | ± 2.7 | ± 2.6 | ± 3.0 | ± 4.2 | ± 6.3 | ± 5.6 | ± 4.9 | ± 2.9 | ± 6.3 | ± 6.7 | ± 2.9 | ± 4.9 | ± 5.3 | ± 4.2 | ± 4.9 | ± 4.8 | ± 8.9 | ± 7.2 |
| range | 73–124 | 73–120 | 40–90 | 90–162 | 91–191 | 74–192 | 94–168 | 47–96 | 76–193 | 75–163 | 45–88 | 85–159 | 105–172 | 99–170 | 93–162 | 51–131 | 58–221 | 79–168 |
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| STE | ± 3.3 | ± 3.5 | ± 3.6 | ± 7.8 | ± 4.6 | ± 8.1 | ± 4.4 | ± 6.3 | ± 10.5 | ± 8.1 | ± 6.3 | ± 10.4 | ± 11.9 | ± 8.3 | ± 6.3 | ± 6.6 | ± 12.8 | ± 6.8 |
| range | 74–97 | 77–100 | 40–67 | 105–148 | 110–139 | 80–133 | 96–125 | 50–87 | 77–150 | 64–118 | 41–86 | 92–165 | 75–159 | 85–143 | 90–125 | 50–88 | 55–151 | 74–118 |
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| STE | ± 2.0 | ± 4.0 | ± 1.5 | ± 8.5 | ± 1.5 | ± 1.5 | ± 5.5 | ± 3.0 | ± 16.0 | ± 4.5 | ± 6.0 | ± 19.0 | ± 0.5 | ± 17.5 | ± 1.5 | ± 0.0 | ± 5.5 | ± 12.5 |
| range | 81–85 | 78–86 | 50–53 | 110–127 | 113–116 | 111–114 | 88–99 | 59–65 | 69–101 | 78–87 | 55–67 | 93–131 | 126–127 | 81–116 | 103–106 | 75–75 | 100–111 | 60–85 |
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| STE | ± 9.3 | ± 10.7 | ± 7.8 | ± 15.9 | ± 18.7 | ± 9.4 | ± 8.8 | ± 6.4 | ± 4.8 | ± 18.2 | ± 14.3 | ± 5.9 | ± 17.9 | ± 4.8 | ± 17.2 | ± 10.4 | ± 8.3 | ± 10.2 |
| range | 81–111 | 66–103 | 54–79 | 112–162 | 118–181 | 114–146 | 104–133 | 43–65 | 94–109 | 66–128 | 36–84 | 115–134 | 93–152 | 105–122 | 80–140 | 51–85 | 107–135 | 84–117 |
Retinal sectors: OD, right eye; OS, left eye; G, global; S, superior; I, inferior; T, temporal; TS, temporal superior; TI, temporal inferior; N, nasal; NS, nasal superior; NI, nasal inferior. All values are given in μm.
Brain atrophy indices in MS patients.
| Group | N = | f:m | age | disease | Evans | CHI | CMI | BCI | maximum | maximum | MFSS | MIF | MSF |
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| width | width | ||||||||||||
| duration | ratio | of 3rd | of 4th | ||||||||||
| ventricle | ventricle | ||||||||||||
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| STE | ± 2.5 | ± 2.5 | ± 0.1 | ± 0.1 | ± 0.2 | ± 0.005 | ± 0.73 | ± 0.37 | ± 0.2 | ± 0.2 | ± 0.2 | ||
| range | 19.75–61.0 | 1.0–45.0 | 0.17–0.34 | 0.05–0.21 | 0.1–0.33 | 0.17–0.25 | 1.5–11.1 | 9.3–14.0 | 1.0–4.1 | 1.5–4.3 | 1.0–5.0 | ||
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| STE | ± 4.0 | ± 4.3 | ± 0.1 | ± 0.1 | ± 0.2 | ± 0.01 | ± 0.59 | ± 0.96 | ± 0.4 | ± 0.3 | ± 0.5 | ||
| range | 19.75–47.5 | 2.0–27.5 | 0.21–0.25 | 0.05–0.12 | 0.07–0.21 | 0.19–0.24 | 1.7–5.2 | 7.3–13.5 | 2.0–4.0 | 1.3–3.4 | 1.0–4.0 | ||
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| STE | ± 9.75 | ± 3.75 | ± 0.1 | ± 0.2 | ± 0.2 | ± 0.04 | ± 1.4 | ± 0.3 | ± 0.7 | ± 0.5 | ± 0.8 | ||
| range | 27.0; 46.5 | 6.5; 14.0 | 0.25–0.27 | 0.10–0.13 | 0.23–0.27 | 0.22–0.31 | 5.9–8.7 | 10.0–10.6 | 2.7–4.1 | 3.3–4.3 | 2.0–3.6 | ||
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| STE | ± 5.2 | ± 5.9 | ± 0.2 | ± 0.1 | ± 0.2 | ± 0.02 | ± 1.72 | ± 1.0 | ± 0.1 | ± 0.4 | ± 0.5 | ||
| range | 30.5–47.5 | 8.5–28.3 | 0.20–0.25 | 0.08–0.12 | 0.12–0.19 | 0.16–0.22 | 3.6–8.9 | 9.4–12.7 | 2.7–3.0 | 1.2–2.5 | 1.4–2.8 |
CHI, the caudate head index; BCI, the basal cistern index; CMI, the cella media index; MIF, the maximum width of the anterior interhemispheric fissure; MSF, the maximum width of the Sylvian fissure; and MFSS, the maximum frontal subarachnoid space.
Fig 1white squares, RRMS without ON; black squares, RRMS with ON; white triangles, SPMS without ON; black triangles, SPMS with ON; black line, linear regression curve. Abbreviations: OD, oculus dexter (right eye); OS, oculus sinister (left eye); RNFL, retinal nerve fiber layer; NAA, N-acetyl-aspartate; Cho, choline; Cr, creatine; NAWM, normal appearing white matter; MIF, the maximum width of the anterior interhemispheric fissure; MSF, the maximum width of the Sylvian fissure; MFSS, the maximum frontal subarachnoid space; EDSS, expanded disability severity scale. a1-g8, linear regression curves for: a1, RNFL vs. NAA (right eye); a2, RNFL vs. NAA (left eye); a3, RNFL vs. Cho (right eye); a4, RNFL vs. Cho (left eye); a5, RNFL vs. Cr (right eye); a6, RNFL vs. Cr (left eye); a7, disease duration vs. NAA in the NAWM; a8, disease duration vs. Cho; b1, RNFL vs. lesion load (right eye); b2, RNFL vs. lesion load (left eye); b3, RNFL vs. lesion load per brain volume (right eye); b4, RNFL vs. lesion load per brain volume (left eye); b5, RNFL vs. lesion load along anterior right visual pathway (right eye); b6, RNFL vs. lesion load anterior right visual pathway (left eye); b7, RNFL vs. lesion load along anterior left visual pathway (right eye); b8, RNFL vs. lesion load anterior left visual pathway (left eye); c1, RNFL vs. lesion load along posterior right visual (right eye); c2, RNFL vs. lesion load along posterior left visual pathway (left eye); c3, RNFL vs. lesion load along posterior left visual (right eye); c4, RNFL vs. lesion load along posterior left visual pathway (left eye); c5, RNFL vs. Evan’s Index (right eye); c6, RNFL vs. Evan’s Index (left eye); c7, RNFL vs. Caudate Head Index (right eye); c8, RNFL vs. Caudate Head Index Index (left eye); d1, RNFL vs. Cella Media Index (right eye); d2, RNFL vs. Cella Media Index (left eye); d3, RNFL vs. Basal Cistern Index (right eye); d4, RNFL vs. Basal Cistern Index Index (left eye); d5, RNFL vs. the maximum width of the 3rd ventricle (right eye); d6, RNFL vs. the maximum width of the 3rd ventricle (left eye); d7, RNFL vs. the maximum of the 4th width ventricle (right eye); d8, RNFL vs. the maximum of the 4th width ventricle (left eye); e1, RNFL vs. MFSS (right eye); e2, RNFL vs. MFSS (left eye); e3, RNFL vs. MIF (right eye); e4, RNFL vs. MIF (left eye); e5, RNFL vs. MSF (right eye); e6, RNFL vs. MSF (left eye); e7, disease duration vs. Evan’s Index; e8, disease duration vs. Caudate Head Index; f1, disease duration vs. Cella Media Index; f2, disease duration vs. the maximum width of the 3rd ventricle; f3, disease duration vs. the maximum width of the 4th ventricle; f4, disease duration vs. MFSS; f5, disease duration vs. MIF; f6, disease duration vs. MSF; f7, disease duration vs. lesion load along both visual pathways; f8, disease duration vs. lesion load along the anterior right visual pathway; g1, disease duration vs. lesion load along the anterior left visual pathway; g2, disease duration vs. lesion load along the posterior right visual pathway; g3, disease duration vs. lesion load along the posterior left visual pathway; g4, disease duration vs. EDSS; g5, disease duration vs. RNFL (right eye); g6, disease duration vs. RNFL (left eye); g7, RNFL (right eye) vs. EDSS; g8, RNFL (right eye) vs. EDSS. Regression analyses demonstrated only weak correlations between the examined parameters a1-g8 of all 28 MS patients included in this study and associated subgroups (RRMS without ON, RRMS with ON, SPMS without ON, SPMS with ON). Of note, the plotted linear regression curves in a1 –g8 are calculated for the analysis of all included MS patient.
Regression Analysis.
Simple regression–linear model: Independent variable, RNFL; dependent variables, NAA, N-acetyl-aspartate; Cho, choline; Cr, creatine; LL per BV, lesionload per Brain Volume, LL AR, lesion load along anterior right visual pathway; LL AL, lesion load along anterior left visual pathway; LL PR, load along posterior right visual pathway; LL PL, load along posterior left visual pathway; Evan’s Index; CHI; CMI; BCI; the maximum width of the 3rd ventricle; the maximum width of the 4th ventricle; MIF, the maximum width of the anterior interhemispheric fissure; MFSS, the maximum frontal subarachnoid space; MSF, the maximum width of the Sylvian fissure; DD, disease duration; EDSS, expanded disability severity scale. 1 row: all right eyes (n = 28; with and without ON) of all included MS patient. 2 row: all left eyes (n = 28; with and without ON) of all included MS patient. 3 row: all right eyes of MS patients who never experienced an ON (neither on their right nor on their left eye; RRMS, n = 17, SPMS, n = 2; Table 1). 4 row: all left eyes of MS patients who never experienced an ON (neither on their left nor on their right eye; RRMS, n = 17, SPMS, n = 2; Table 1). Patients are the same as in the 3rd row. 5 row: right eyes of 6 MS patients who experienced an ON on their right eyes (note, 4 out of 6 experienced ON on both eyes, 2 only on their right eyes; Table 1). 6 row: left eyes of 6 MS patients who experienced an ON on their left eyes (note, 4 out of 7 experienced ON on both eyes, 3 only on their left eyes Table 1). For each analysis the correlation coefficient (corr. coeff.), R-squared (percent), the standard error of estimate (STE of Est.) and the p-value (analysis of variance, ANOVA) is given. Since the p-value in the ANOVA table is less than 0.01, there is a statistically significant relationship between the maximum width of the 4th ventricle and the RNFL (for all patients’ right eyes, n = 28, 1st row and for all patient’s left eyes, who never experienced ON, n = 17, 4th row) at 99% confidence level. However, the low correlation coefficient indicates that there is only a weak relationship between the variables. R-squared statistic indicates that the simple/linear regression explains only 24.92% (1st row) or 28.68% (4th row) of the variability of the independent variable. In all other analyses presented here (and performed for the six OCT-Sectors, see material and methods or Table 5) no statistically significant correlation could be found (data not shown).
| RNFL | NAA | Cho | Cr | LL, per | LL, AR | LL, AL | LL, PR | LL, PL | Evans | CHI | CMI | BCI | width | width | MFSS | MIF | DD | EDSS | |
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| BV | ratio | of 3rd | of 4th | ||||||||||||||||
| ventricle | ventricle | ||||||||||||||||||
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| R-squared | 0.17 | 0.35 | 1.87 | 2.30 | 0.01 | 5.79 | 0.088 | 0.712 | 0.450 | 1.527 | 5.616 | 1.785 | 12.1 | 24.29 | 3.511 | 0.371 | 4.17 | 7.28 |
| STE of Est. | 2.41 | 0.36 | 1.12 | 0.58 | 168 | 123 | 566.2 | 451 | 0.05 | 0.04 | 0.07 | 0.02 | 2.63 | 1.463 | 0.79 | 0.87 | 7.11 | 1.71 | |
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| R-squared | 1.32 | 0.58 | 2.26 | 5.76 | 4.05 | 9.81 | 4.12 | 6.63 | 0.19 | 0.57 | 0.81 | 0.19 | 2.26 | 21.40 | 0.86 | 0.84 | 9.77 | 13.97 |
| STE of Est. | 2.42 | 0.36 | 1.12 | 0.57 | 164.9 | 120.8 | 554.7 | 437.6 | 0.05 | 0.04 | 0.07 | 0.02 | 2.78 | 1.49 | 0.80 | 0.87 | 6.90 | 1.65 | |
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| R-squared | 2.30 | 0.23 | 9.76 | 0.01 | 0.47 | 1.23 | 0.19 | 1.05 | 4.01 | 0.40 | 8.86 | 3.52 | 10.88 | 14.92 | 6.89 | 0.09 | 6.13 | 2.63 |
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| STE of Est. | 2.44 | 0.42 | 1.21 | 0.54 | 119.2 | 125,0 | 525,3 | 334.8 | 0.05 | 0.04 | 0.07 | 0.02 | 2.86 | 1,40 | 0.75 | 0.93 | 7.39 | 1.29 |
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| R-squared | 6.60 | 0.60 | 11.26 | 0.001 | 0.36 | 0.69 | 0.07 | 0.10 | 5.45 | 0.54 | 5.97 | 0.03 | 3.93 | 28.68 | 6.26 | 0.75 | 14.94 | 5.16 |
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| STE of Est. | 2.39 | 0.43 | 1.19 | 0.53 | 120,59 | 125,38 | 525.60 | 336,47 | 0.05 | 0.04 | 0.07 | 0.02 | 2.97 | 1.28 | 0.75 | 0.94 | 7.04 | 1.27 |
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| R-squared | 16.60 | 1.60 | 0.59 | 0.87 | 15.01 | 9.12 | 7.69 | 8.57 | 11.12 | 4.87 | 11.12 | 11.12 | 1.15 | 46.92 | 14.89 | 1.78 | 47.21 | 47.65 |
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| STE of Est. | 2.06 | 2.32 | 0.63 | 0.41 | 241.75 | 119.20 | 433.31 | 349.74 | 0.04 | 0.04 | 0.04 | 0.04 | 1.15 | 1.47 | 0.86 | 0.92 | 3.41 | 2.04 |
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| R-squared | 6.84 | 30.26 | 26.49 | 12.59 | 1.80 | 39.26 | 13.09 | 8.18 | 14.99 | 5.59 | 18.18 | 1.56 | 9.53 | 43.87 | 1.66 | 0.17 | 15.44 | 25.35 |
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| STE of Est. | 2.95 | 0.15 | 0.82 | 0.72 | 255.51 | 101.97 | 628.24 | 681.43 | 0.039 | 0.04 | 0.04 | 0.04 | 2.49 | 1.67 | 0.92 | 0.72 | 7.36 | 2.25 |
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Fig 2CROP, Clinico-Radiologico-Ophthalmological Paradox in MS.
MRI, 3 Tesla, serial sections: 1st row, sagittal, 2nd row, axial and 3rd row, coronar images from a RRMS patient with rather long disease course and highly active disease. Although very high lesion load in the whole brain and visual pathway and obvious brain atrophy the patient had normal RNFL and TMV values. (patient 1, Table 1).
Metabolites in NAWM and lesion load in the visual pathways in MS patients.
| Metabolites in NAWM | lesion volume in visual pathway | |||||||||||
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| Group | N = | f:m | age | disease | Cho | Cr[mM] | NAA[mM] | AD/ | AS/ | PD/ | PS/ | Total |
| duration | [mM] | [mM] | [mM] | Volume | Volume | Volume | Volume | Lesion/ | ||||
| Volume | ||||||||||||
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| STE | ± 2.5 | ± 2.5 | ± 0.10 | ± 0.30 | ± 0.60 | ± 0.02 | ± 0.02 | ± 0.09 | ± 0.08 | ± 0.2 | ||
| range | 19.75–61.0 | 1.0–45.0 | 1.47–3.15 | 4.72–10.55 | 4.86–14.08 | 0.00–0.28 | 0.00–0.23 | 0.01–1.39 | 0.02–1.22 | 0.03–2.71 | ||
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| STE | ± 4.0 | ± 4.3 | ± 0.07 | ± 0.44 | ± 1.09 | ± 0.06 | ± 0.05 | ± 0.20 | ± 0.23 | ± 0.51 | ||
| range | 19.75–47.5 | 2.0–27.5 | 2.11–2.58 | 6.48–9.48 | 7.67–14.95 | 0.00–0.33 | 0.00–0.28 | 0.19–1.48 | 0.10–1.47 | 0.32–3.54 | ||
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| STE | ± 9.75 | ± 3.75 | ± 0.28 | ± 0.45 | ± 0.73 | ± 0.10 | ± 0.10 | ± 0.54 | ± 0.06 | ± 0.80 | ||
| range | 27.0; 46.5 | 6.5; 14.0 | 1.91–2.48 | 6.91–7.81 | 9.14–10.59 | 0.20–0.40 | 0.23–0.42 | 1.04–2.12 | 0.90–1.02 | 2.37; 3.54 | ||
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| STE | ± 5.2 | ± 5.9 | ± 0.11 | ± 0.21 | ± 0.81 | ± 0.13 | ± 0.06 | ± 0.23 | ± 0.34 | ± 0.69 | ||
| range | 30.5–47.5 | 8.5–28.3 | 2.40–2.76 | 8.11–8.77 | 8.25–11.07 | 0.05–0.49 | 0.04–0.24 | 0.78–1.48 | 0.48–1.60 | 1.36–3.70 | ||
Metabolites, N-Acetyl-Aspartate (NAA), Choline (Cho) and creatine (Cr) given in mM; lesion load in the visual pathways, here given as ratio of lesion volume in the visual pathways (AD, right anterior; AS, left anterior; PD, right posterior; PS, left posterior and total lesion volume) to total brain volume.
RNFL and TMV in MS patients, global.
| Group | N = | f:m | age | disease | RNFL, | RNFL, | TMV, | TMV, |
|---|---|---|---|---|---|---|---|---|
| duration | global OD | global OS | OD | OS | ||||
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| STE | ± 2.5 | ± 2.5 | ± 2.70 | ± 0.2.68 | ± 0.12 | ± 0.14 | ||
| range | 19.75–61.0 | 1.0–45.0 | 73.0–124.0 | 73.0–120.0 | 7.71–9.39 | 7.32–9.43 | ||
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| STE | ± 4.0 | ± 4.3 | ± 3.27 | ± 3.48 | ± 0.23 | ± 0.20 | ||
| range | 19.75–47.5 | 2.0–27.5 | 74.0–97.0 | 77.0–100.0 | 7.47–9.02 | 7.82–9.15 | ||
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| STE | ± 9.75 | ± 3.75 | ± 2.00 | ± 4.00 | ± 0.11 | ± 0.32 | ||
| range | 27.0; 46.5 | 6.5; 14.0 | 81.0–85.0 | 78.0–86.0 | 8.04–8.26 | 8.19–8.83 | ||
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| STE | ± 5.2 | ± 5.9 | ± 9.28 | ± 10.71 | ± 0.05 | ± 0.36 | ||
| range | 30.5–47.5 | 8.5–28.3 | 81.0–111.0 | 66.0–103.0 | 8.01–8.18 | 7.33–8.57 |
OD, right eye; OS, left eye. All RNFL values are given in μm. All TMV values are given in mm .