Detailed exploration of studies evaluating the use of highly effective treatments have unveiled the clinical concept of Progression Independent of disease activity (PIRA), or an accumulation of disability in the absence of relapse-associated worsening (RAW), in multiple sclerosis (MS).
It has become something of a hot topic in research and clinical practice in recent years, but many questions remain surrounding its frequency, pathological determinants, treatment, and implications.
During our second NeuroWebinar in May, Professor Alan Thompson, Dean of the Faculty of Brain Sciences at University College London and editor of the Multiple Sclerosis Journal, Dr Carmen Tur, Neurologist at the Multiple Sclerosis Centre of Catalonia (CEMCAT), and Professor Cristina Granziera, Senior Consultant Neurologist at the University Hospital of Basel, discussed the growing evidence base, the latest research on and around PIRA, and how they expect it to affect clinical practice.
An emerging area of interest
PIRA events, said Prof Thompson, can occur from the earliest stages of MS, are an important driver of cumulative disability in the long term, and are associated with underlying brain and spinal cord atrophy.
“As such, many suggest it is the result of accumulating damage from multiple, yet only partially understood, pathological mechanisms across the disease course,” he added. “It may also be associated with inflammatory activity on MRI, but the impact of age, disease duration, co-morbidities, and exposure to disease modifying treatments (DMTs), have all yet to be clearly established.”
Frequency, predictability, and prognosis
The evidence suggests PIRA is relatively frequent, said Dr Tur, who led a Spanish study that followed 1,000-plus people for more than 25 years after a first demyelinating event, or clinically isolated syndrome. Around 25% of the cohort experienced PIRA, with the first event occurring at a median time of approximately seven years post-CIS.[1]
Analysis of the data found older age at the time of CIS was the only strong predictor of PIRA. A higher number of brain lesions and the presence of spinal cord lesions conferred a higher risk of earlier PIRA, said Dr Tur.
Prof Granziera’s team investigated the question of whether PIRA was associated with accelerated brain tissue loss. They found that, in a cohort of more than 500 people with relapsing MS (RMS), those with PIRA exhibited accelerated brain atrophy, especially in the cerebral cortex.[2]
Dr Tur’s study also found that patients who experienced a PIRA event within the first five years post-CIS had a more than 20 times higher risk of reaching Expanded Disability Status Score (EDSS) six, when compared to those with a later PIRA.[1]
“Those patients with an early PIRA event also had steeper curves of EDSS increase over time… an early PIRA event was associated with a greater risk of unfavourable outcomes,” she said, adding that those with an earlier PIRA event were older and had a higher number of spinal cord lesions.
Prof Granziera agreed that a higher number of spinal cord lesions at disease onset was likely to be a predictive of worse outcomes. “I think this points us to the necessity of monitoring these patients in a different way,” she said. “As a community, we need to think about our recommendations for extensive spinal cord examination during the first year of the disease.”
Pathological determinants and possible treatment
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