Falls, functioning, and disability among women with persistent symptoms of chemotherapy-induced peripheral neuropathy

Winters-Stone, Kerri M.; Horak, Fay Bahling; Jacobs, Peter G.; Trubowitz, Phoebe; Dieckmann, Nathan F.; Stoyles, Sydnee; Faithfull, Sara

doi:10.1200/JCO.2016.71.3552

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Falls, functioning, and disability among women with persistent symptoms of chemotherapy-induced peripheral neuropathy
Citation	Winters-Stone KM, Horak FB, Jacobs PG, Trubowitz P, Dieckmann NF, Stoyles S, Faithfull S. J. Clin. Oncol. 2017; 35(23): 2604-2612.
Affiliation	Kerri M. Winters-Stone, Fay Horak, Peter G. Jacobs, Phoebe Trubowitz, Nathan F. Dieckmann, and Sydnee Stoyles, Oregon Health & Science University, Portland, OR; and Sara Faithfull, University of Surrey, Guildford, Surrey, United Kingdom.
Copyright	(Copyright © 2017, American Society of Clinical Oncology)
DOI	10.1200/JCO.2016.71.3552
PMID	28586243
Abstract	PURPOSE Chemotherapy-induced peripheral neuropathy (CIPN) may persist after treatment ends and may lead to functional decline and falls. This study compared objective and self-report measures of physical function, gait patterns, and falls between women cancer survivors with and without symptoms of CIPN to identify targets for functional rehabilitation. METHODS A secondary data analysis of 512 women cancer survivors (age, 62 ± 6 years; time since diagnosis, 5.8 ± 4.1 years) categorized and compared women self-reporting symptoms of CIPN (CIPN+) with asymptomatic women (CIPN-) on the following: maximal leg strength, timed chair stand, physical function battery, gait characteristics (speed; step number, rate, and length; base of support), self-report physical function and disability, and falls in the past year. RESULTS After an average of 6 years after treatment, 47% of women still reported symptoms of CIPN. CIPN+ had significantly worse self-report and objectively measured function than did CIPN-, with the exception of maximal leg strength and base of support during a usual walk. Gait was slower among CIPN+, with those women taking significantly more, but slower and shorter, steps than did CIPN- (all P <.05). CIPN+ reported significantly more disability and 1.8 times the risk of falls compared with CIPN- ( P <.0001). Increasing symptom severity was linearly associated with worsening function, increasing disability, and higher fall risk (all P <.05). CONCLUSION This work makes a significant contribution toward understanding the functional impact of CIPN symptoms on cancer survivors. Remarkably, 47% of women in our sample had CIPN symptoms many years after treatment, together with worse function, greater disability, and more falls. CIPN must be assessed earlier in the clinical pathway, and strategies to limit symptom progression and to improve function must be included in clinical and survivorship care plans. Language: en