image: Antibody administration following saline or BTX administration at the beginning of the treatment. Anti-IGF1R antibody treatment is denoted as IGF1R and control IgG antibody treatment as control IgG. Data is presented as mean + standard deviation. *P0.05, ***P0.001, ****P0.0001, and P0.01 were calculated using two-way ANOVA followed by a Tukey's test.
Credit: Prof. Masashi Fujitani from Shimane University, Japan (https://www.nature.com/articles/s41419-023-06128-w#Fig1)
Botulinum toxin-A (BTX), also known as Botox®, is used to treat a range of neuromuscular disorders, including muscle spasms, dystonia, eye twitching, overactive bladder, and spasticity associated with cerebral palsy or stroke. Notably, BTX has gained popularity in cosmetology owing to its effectiveness in minimizing facial wrinkles. BTX works by inducing paralysis at neuromuscular junctions (NMJs) — the connections between a neuron (brain cell) and a muscle fiber. However, owing to the gradual recovery of NMJs, BTX has a relatively short duration of action. Patients require repeated BTX injections at short intervals, which limits the accessibility of BTX to patients. Hence, strategies to improve the duration of BTX’s therapeutic benefits would be extremely useful.
This feat has now been made possible by a research group led by Prof. Masashi Fujitani from the Department of Anatomy and Neuroscience, Faculty of Medicine, Shimane University, Japan. In a study published in the renowned journal Cell Death & Disease on 16 September 2023, the team, which also comprised Dr. Hiroki Ishihara, Dr. Yoshinori Otani, Dr. Hisao Miyajima, and Dr. Huy Xuan Ngo from Shimane University, demonstrates that the paralytic effect of BTX at the NMJ can be prolonged by specifically blocking the insulin-like growth factor 1 receptor (IGF1R) — a cell surface protein involved in NMJ regeneration. “Given that BTX specifically targets NMJs, we sought to understand if its paralytic therapeutic effects could be prolonged by preventing NMJ regeneration. To do this, we targeted regenerative factors that support NMJ regeneration and zeroed in on IGF1R,” explains Prof. Fujitani.
This study was conducted using a mouse model. Specifically, the researchers focused on the gastrocnemius (GC) muscle in the leg. After BTX treatment, they blocked IGF1R in this muscle using an intramuscular injection of a specific anti-IGF1R antibody. Subsequently, the experimental mice were subjected to a variety of tests, including footprint and gait analysis, to examine the effect of IGF1R blockade. The muscle tissue was also dissected to perform morphological analysis and study changes at the NMJ.
The results of this study showed that blocking IGF1R could slow down recovery from BTX-induced paralysis, thereby extending the therapeutic effects of BTX. This was accompanied by biological alterations at the NMJ. On exploring the molecular mechanisms underlying this effect, the researchers found that NMJ regeneration following BTX treatment was mediated by translation signaling via the mTOR/S6 kinase signaling pathway, which is the key controller of mammalian metabolism and physiology. However, anti-IGF1R antibodies inhibited this pathway, thereby impairing regeneration and prolonging the therapeutic benefits of BTX.
To Prof. Fujitani and the rest of his research group, these results signify a major milestone in BTX therapy and herald a bright future for the management of neuromuscular disorders. “In clinical settings, IGF1R inhibition could decrease the number of injections and the total dose of BTX necessary by prolonging the duration of its effects. This would be especially crucial in the areas of rehabilitation and cosmetic therapy, where patients seek sustained results. We are now looking at a significant reduction in the cost and burden of BTX, which can impact a large group of patients,” comments Prof. Fujitani.
Indeed, the new BTX therapy in combination with anti-IGF1R treatment could provide more long-lasting results, allowing patients to experience prolonged benefits. It could reduce the number of BTX treatment sessions required, making the treatment more cost-effective, reducing hospital visits, and potentially increasing patient convenience and adherence. Most importantly, it provides a major source of hope for the many patients who may benefit from it in the future.
About Shimane University
Shimane University’s Faculty of Medicine is located in Izumo City and was formed as a result of a merger with Shimane University in 2003. Since its establishment, the faculty has produced 4,798 graduates who are functioning in a wide variety of capacities within and outside Japan. The faculty strives to produce individuals who are committed to a career in community medicine, education, and medical research. Its mission is to instill qualities such as knowledge, problem-solving ability, communicative competence, and professionalism in its students, as well as to advance basic and clinical research towards the benefit of the society.
Website: https://www.med.shimane-u.ac.jp/
About Professor Masashi Fujitani from Shimane University
Masashi Fujitani is a Professor in the Faculty of Medicine at Shimane University, Japan. He obtained his doctorate from the Shiga University of Medical Science and has since dedicated his research career to exploring the pathology and treatment of neurological disorders. Specifically, his interest lies in the areas of neurodevelopmental disorders, neuroimmune diseases, and axon regeneration. His rigorous work and expertise have earned him over 60 publications in well-reputed international journals.
Website: https://www.fujitani-lab.net/
Journal
Cell Death and Disease
Method of Research
Experimental study
Subject of Research
Animals
Article Title
Blocking insulin-like growth factor 1 receptor signaling pathway inhibits neuromuscular junction regeneration after botulinum toxin-A treatment
Article Publication Date
16-Sep-2023
COI Statement
The authors declare no competing interests