Onset of secondary progressive multiple sclerosis is not influenced by current relapsing multiple sclerosis therapies

Coret, Francisco; Pérez‐Miralles, Francisco; Gascón, Francisco; Alcalá, Carmen; Navarré, Arantxa; Bernad, Ana; Boscá, Isabel; Escutia, M. Pérez; Gil-Perotín, Sara; Casanova, Bonaventura

doi:10.1177/2055217318783347

Cited by 24 publications

(30 citation statements)

References 39 publications

(76 reference statements)

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“…]” This concept implies the hypothesis that two different clinical forms of MS could coexist from the beginning of the disease: one with a relapsing debut, in which progressive MS will never develop, and the other with a relapsing course, but with a silent progression from the beginning, responsible for the subsequent progressive course of SPMS. Similar data were published by our group in a cohort of 204 RRMS patients followed for 20 years, work in which we discussed the concept of bout onset progressive MS (BOPMS), first mentioned by Paz Soldán et al…”

supporting

confidence: 82%

Silent Progression or Bout Onset Progressive Multiple Sclerosis?

Gil-Perotín

Alcalá

Pérez‐Miralles

et al. 2019

Annals of Neurology

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Recently, Cree et al 1 coined the term "silent progression" to emphasize the existence of progression of disability in patients who suffer from a relapsing form of multiple sclerosis (MS). In their work, 20% of patients developed a secondary progressive form of MS (SPMS) after a mean evolution time of 20 years. Interestingly, neither early relapses nor treatment influenced the likelihood of long-term disability. The authors suggest that the same underlying process that causes a silent progression during the relapsing phase of MS is responsible for the characteristic disease course in SPMS, and they emphasized, "that it is not an invariable accompaniment of RRMS [relapsing-remitting multiple sclerosis.]" This concept implies the hypothesis that two different clinical forms of MS could coexist from the beginning of the disease: one with a relapsing debut, in which progressive MS will never develop, and the other with a relapsing course, but with a silent progression from the beginning, responsible for the subsequent progressive course of SPMS. Similar data were published by our group in a cohort of 204 RRMS patients followed for 20 years, 2 work in which we discussed the concept of bout onset progressive MS (BOPMS), first mentioned by Paz Soldán et al. 3 We would like to ask Cree et al about two concerns. The first is whether they consider that the group of relapsing MS patients with silent progression is the same as the one previously defined as BOPMS; and the second is, if these groups are not considered the same, what are the differences between them?Along these lines, we believe that introducing a new concept to define progression in the relapsing phase of MS could possibly cause more confusion in the definition of MS course. In our opinion, the BOPMS concept properly reflects the idea of the existence of a continuum between the relapsing phase, with an underlying silent progression, and SPMS. The BOPMS concept also links the two progressive forms of MS, SPMS and the primary progressive MS, under the same category, highlighting that progression is a common mechanism to both forms of progressive MS, regardless of whether there were relapses at the beginning of the disease.Nothing to report.

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supporting

confidence: 82%

Silent Progression or Bout Onset Progressive Multiple Sclerosis?

Gil-Perotín

Alcalá

Pérez‐Miralles

et al. 2019

Annals of Neurology

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“…Research into how this transition can be prevented is therefore of vital importance. Disease course is often unpredictable, and the underlying mechanisms behind why some RR MS patients progress to SP MS and others do not is incompletely understood133 . The effect of MS DMD's once the progressive phase has been reached is less clear than is the case for RR MS, highlighting the importance of preventing transition to SP MS since treatments cannot necessarily be depended on to alleviate symptoms to the same degree134 .…”

mentioning

confidence: 99%

The association between multiple sclerosis and pain medications

Burkill

Montgomery

Kockum

et al. 2018

PAIN

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“…Naturally, certain risk factors have been described, which could suggest or predict the manifestation of secondary progression in MS patients. Among the demographic characteristics of the patients at the RRMS diagnosis, male sex ( 29 , 33 – 35 ), older age ( 21 , 29 , 35 – 38 ), and a multifocal disease manifestation at onset ( 36 , 37 ) have been associated with an earlier transition to SPMS. Regarding the disease course, patients with a low EDSS at MS diagnosis could have a lower risk of disability progression further on ( 36 ); the annual relapse rate may be a predictive factor especially in the earlier disease stages ( 27 , 29 , 35 , 36 ).…”

Section: Pathophysiology Of Disease Progressionmentioning

confidence: 99%

“…The use of DMTs seems to modify the risk of a secondary progressive course. First-line DMTs may prolong the period to transition to SPMS according to several studies ( 18 , 19 , 29 , 36 ), although a lack of an objective influence has also been suggested ( 37 , 41 ). Furthermore, the use of newer high-effective DMTs is associated with an even lower risk of disability accumulation compared to the first-line therapies ( 19 ).…”

Section: Pathophysiology Of Disease Progressionmentioning

confidence: 99%

Should We Use Clinical Tools to Identify Disease Progression?

et al. 2021

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The presence of disability progression in multiple sclerosis (MS) is an important hallmark for MS patients in the course of their disease. The transition from relapsing remitting (RRMS) to secondary progressive forms of the disease (SPMS) represents a significant change in their quality of life and perception of the disease. It could also be a therapeutic key for opportunities, where approaches different from those in the initial phases of the disease can be adopted. The characterization of structural biomarkers (e.g., magnetic resonance imaging or neurofilament light chain) has been proposed to differentiate between both phenotypes. However, there is no definite threshold between them. Whether the risk of clinical progression can be predicted by structural markers at early disease phases is still a focus of clinical research. However, several theories and pathological evidence suggest that both disease phenotypes are part of a continuum with common pathophysiological mechanisms. In this case, the clinical evaluation of the patients would play a preponderant role above destruction biomarkers for the early identification of disability progression and SPMS. For this purpose, the use of clinical tools beyond the Expanded Disability Status Scale (EDSS) should be considered. Besides established functional tests such as the Multiple Sclerosis Functional Composite (MSFC), patient's neurological history or digital resources may help neurologists in the decision-taking. In this article, we discuss arguments for the use of clinical markers in the detection of secondary progressive MS and the characterization of progressive disease activity.

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Onset of secondary progressive multiple sclerosis is not influenced by current relapsing multiple sclerosis therapies

Cited by 24 publications

References 39 publications

Silent Progression or Bout Onset Progressive Multiple Sclerosis?

Silent Progression or Bout Onset Progressive Multiple Sclerosis?

The association between multiple sclerosis and pain medications

Should We Use Clinical Tools to Identify Disease Progression?

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