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Systemic inflammation associates with and precedes cord atrophy in progressive multiple sclerosis

Systemic inflammation associates with and precedes cord atrophy in progressive multiple sclerosis
Systemic inflammation associates with and precedes cord atrophy in progressive multiple sclerosis

In preclinical models of multiple sclerosis, systemic inflammation has an impact on the compartmentalized inflammatory process within the central nervous system and results in axonal loss. It remains to be shown whether this is the case in humans, specifically whether systemic inflammation contributes to spinal cord or brain atrophy in multiple sclerosis. Hence, an observational longitudinal study was conducted to delineate the relationship between systemic inflammation and atrophy using magnetic resonance imaging: the SIMS (Systemic Inflammation in Multiple Sclerosis) study. Systemic inflammation and progression were assessed in people with progressive multiple sclerosis ( n = 50) over two and a half years. Eligibility criteria included: (i) primary or secondary progressive multiple sclerosis; (ii) age ≤ 70; and (iii) Expanded Disability Status Scale ≤ 6.5. First morning urine was collected weekly to quantify systemic inflammation by measuring the urinary neopterin-to-creatinine ratio using a validated ultra-performance liquid chromatography mass spectrometry technique. The urinary neopterin-to-creatinine ratio temporal profile was characterized by short-term responses overlaid on a background level of inflammation, so these two distinct processes were considered as separate variables: background inflammation and inflammatory response. Participants underwent MRI at the start and end of the study, to measure cervical spinal cord and brain atrophy. Brain and cervical cord atrophy occurred on the study, but the most striking change was seen in the cervical spinal cord, in keeping with the corticospinal tract involvement that is typical of progressive disease. Systemic inflammation predicted cervical cord atrophy. An association with brain atrophy was not observed in this cohort. A time lag between systemic inflammation and cord atrophy was evident, suggesting but not proving causation. The association of the inflammatory response with cord atrophy depended on the level of background inflammation, in keeping with experimental data in preclinical models where the effects of a systemic inflammatory challenge on tissue injury depended on prior exposure to inflammation. A higher inflammatory response was associated with accelerated cord atrophy in the presence of background systemic inflammation below the median for the study population. Higher background inflammation, while associated with cervical cord atrophy itself, subdued the association of the inflammatory response with cord atrophy. Findings were robust to sensitivity analyses adjusting for potential confounders and excluding cases with new lesion formation. In conclusion, systemic inflammation associates with, and precedes, multiple sclerosis progression. Further work is needed to prove causation since targeting systemic inflammation may offer novel treatment strategies for slowing neurodegeneration in multiple sclerosis.

multiple sclerosis, progression, systemic inflammation
2632-1297
Stuart, Charlotte M.
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Varatharaj, Aravinthan
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Zou, Yukai
328b4fd9-da35-42bb-a032-b0a98ed33a2d
Darekar, Angela
e66f3c01-0825-4da9-af68-e645f4c57f62
Domjan, Janine
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Gandini Wheeler-Kingshott, Claudia A M
fc80a119-935e-42f0-b352-cb2e57055272
Perry, V. Hugh
8f29d36a-8e1f-4082-8700-09483bbaeae4
Galea, Ian
66209a2f-f7e6-4d63-afe4-e9299f156f0b
Stuart, Charlotte M.
734d13d9-fd1f-4c55-ba90-bf1abf303bb4
Varatharaj, Aravinthan
33d833af-9459-4b21-8489-ce9c0b6a09e0
Zou, Yukai
328b4fd9-da35-42bb-a032-b0a98ed33a2d
Darekar, Angela
e66f3c01-0825-4da9-af68-e645f4c57f62
Domjan, Janine
d9283626-a32f-4bae-83ba-699395906305
Gandini Wheeler-Kingshott, Claudia A M
fc80a119-935e-42f0-b352-cb2e57055272
Perry, V. Hugh
8f29d36a-8e1f-4082-8700-09483bbaeae4
Galea, Ian
66209a2f-f7e6-4d63-afe4-e9299f156f0b

Stuart, Charlotte M., Varatharaj, Aravinthan, Zou, Yukai, Darekar, Angela, Domjan, Janine, Gandini Wheeler-Kingshott, Claudia A M, Perry, V. Hugh and Galea, Ian (2024) Systemic inflammation associates with and precedes cord atrophy in progressive multiple sclerosis. Brain Communications, 6 (3), [fcae143]. (doi:10.1093/braincomms/fcae143).

Record type: Article

Abstract

In preclinical models of multiple sclerosis, systemic inflammation has an impact on the compartmentalized inflammatory process within the central nervous system and results in axonal loss. It remains to be shown whether this is the case in humans, specifically whether systemic inflammation contributes to spinal cord or brain atrophy in multiple sclerosis. Hence, an observational longitudinal study was conducted to delineate the relationship between systemic inflammation and atrophy using magnetic resonance imaging: the SIMS (Systemic Inflammation in Multiple Sclerosis) study. Systemic inflammation and progression were assessed in people with progressive multiple sclerosis ( n = 50) over two and a half years. Eligibility criteria included: (i) primary or secondary progressive multiple sclerosis; (ii) age ≤ 70; and (iii) Expanded Disability Status Scale ≤ 6.5. First morning urine was collected weekly to quantify systemic inflammation by measuring the urinary neopterin-to-creatinine ratio using a validated ultra-performance liquid chromatography mass spectrometry technique. The urinary neopterin-to-creatinine ratio temporal profile was characterized by short-term responses overlaid on a background level of inflammation, so these two distinct processes were considered as separate variables: background inflammation and inflammatory response. Participants underwent MRI at the start and end of the study, to measure cervical spinal cord and brain atrophy. Brain and cervical cord atrophy occurred on the study, but the most striking change was seen in the cervical spinal cord, in keeping with the corticospinal tract involvement that is typical of progressive disease. Systemic inflammation predicted cervical cord atrophy. An association with brain atrophy was not observed in this cohort. A time lag between systemic inflammation and cord atrophy was evident, suggesting but not proving causation. The association of the inflammatory response with cord atrophy depended on the level of background inflammation, in keeping with experimental data in preclinical models where the effects of a systemic inflammatory challenge on tissue injury depended on prior exposure to inflammation. A higher inflammatory response was associated with accelerated cord atrophy in the presence of background systemic inflammation below the median for the study population. Higher background inflammation, while associated with cervical cord atrophy itself, subdued the association of the inflammatory response with cord atrophy. Findings were robust to sensitivity analyses adjusting for potential confounders and excluding cases with new lesion formation. In conclusion, systemic inflammation associates with, and precedes, multiple sclerosis progression. Further work is needed to prove causation since targeting systemic inflammation may offer novel treatment strategies for slowing neurodegeneration in multiple sclerosis.

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Accepted/In Press date: 17 April 2024
Published date: 20 April 2024
Keywords: multiple sclerosis, progression, systemic inflammation

Identifiers

Local EPrints ID: 490041
URI: http://eprints.soton.ac.uk/id/eprint/490041
ISSN: 2632-1297
PURE UUID: d161051f-d8c1-4cf2-bd48-1f47c43d6563
ORCID for Charlotte M. Stuart: ORCID iD orcid.org/0000-0002-5779-5487
ORCID for Aravinthan Varatharaj: ORCID iD orcid.org/0000-0003-1629-5774
ORCID for Yukai Zou: ORCID iD orcid.org/0000-0002-9924-5926
ORCID for Ian Galea: ORCID iD orcid.org/0000-0002-1268-5102

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Date deposited: 14 May 2024 16:30
Last modified: 13 Jun 2024 01:59

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Contributors

Author: Charlotte M. Stuart ORCID iD
Author: Yukai Zou ORCID iD
Author: Angela Darekar
Author: Janine Domjan
Author: Claudia A M Gandini Wheeler-Kingshott
Author: V. Hugh Perry
Author: Ian Galea ORCID iD

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