Systemic cancer treatment linked to 5% skeletal muscle loss over 90 days

Photo by julien Tromeur / Unsplash

Acta oncologica (Stockholm, Sweden) Published June 3, 2026 Medically reviewed June 3, 2026 Study authors: Svendsen Lukas, Jensen Sandra, Hansen Stine, Sørensen Victor, Johansen Christoffer, Suetta Charlotte… PubMed ↗ DOI ↗ By Dr. Julia Lee, PhD · Oncology, Genomics & Drug Development

Key Takeaway

Consider monitoring skeletal muscle mass in cancer patients on systemic therapy; average loss is 5% over 90 days.

This systematic review and meta-analysis examined the association between systemic cancer treatment and changes in skeletal muscle mass (SMM) in patients with cancer. The analysis included 78 studies with a total of 10,502 patients receiving chemotherapy and/or immunotherapy, with or without targeted therapy. The median interval between assessments was 90 days (IQR: 71-129). No comparator group was included; the analysis focused on longitudinal change within patients.

The primary outcome was change in SMM during systemic cancer treatment. The pooled standardized mean change (SMC) was -0.24 (95% CI: -0.29 to -0.20), indicating a small decline in muscle mass. This corresponds to an absolute loss of approximately 5% over the median 90-day interval. The effect size is considered small according to Cohen's thresholds.

No secondary outcomes were reported in the meta-analysis. Safety and tolerability data, including adverse events, serious adverse events, and discontinuations, were not reported. The review did not assess clinical outcomes such as survival, quality of life, or treatment toxicity.

Compared to prior literature, this finding aligns with known catabolic effects of cancer and its treatments, but the high heterogeneity (I²=92%) suggests that the true effect varies considerably across studies. This limits the interpretability of a single pooled estimate. The authors note that prospective studies with standardized methods are needed to better characterize muscle loss.

Key methodological limitations include substantial heterogeneity, lack of a comparator group, and reliance on observational data. The pooled estimate represents an association, not causation. Effect sizes were generally small, and the clinical significance of a 5% loss over 90 days may vary by patient population.

For clinical practice, these results suggest that muscle loss is a measurable consequence of systemic cancer treatment, though the magnitude is modest on average. Clinicians should consider monitoring SMM in patients undergoing treatment, especially those at risk for sarcopenia. However, the high heterogeneity means individual patient trajectories may differ substantially.

Unanswered questions include the impact of specific treatment regimens, the role of targeted therapies, the relationship between muscle loss and clinical outcomes, and whether interventions such as exercise or nutrition can mitigate this decline. Future research should focus on standardized assessment methods and prospective designs.

Study Details

Study typeMeta analysis

Sample sizen = 10,502

EvidenceLevel 1

Follow-up768.0 mo

PublishedMay 2026

PMID42200373

View Original Abstract ↓

BACKGROUND AND PURPOSE: Loss of skeletal muscle mass (SMM) is common during systemic cancer treatment, but the magnitude and variability across cancer and treatment types remain uncertain. We aimed to describe changes in SMM during systemic cancer treatment supported by pooled quantitative estimates. PATIENTS/MATERIAL AND METHODS: We systematically searched PubMed, Embase, and Web of Science until April 2025 for longitudinal studies reporting SMM during chemotherapy and/or immunotherapy (± targeted therapy) in patients with cancer (PROSPERO CRD42022308388). Standardized mean changes (SMC) were pooled in random-effects meta-analyses using the restricted maximum-likelihood estimator with Hartung-Knapp adjustment. Heterogeneity was assessed using I². Risk of bias was assessed with the NIH Quality Assessment Tool for Observational Cohort and Cross-Sectional Studies. RESULTS: Seventy-eight studies (n = 10,502; 52% male; median age 64 years [interquartile range, IQR: 34-77]) were included. Meta-analysis across cancers showed an association between systemic cancer treatment and decline in SMM (59 studies; n = 6,373; SMC = -0.24, 95% confidence interval [CI]: -0.29 to -0.20; I² = 92%), corresponding to -5% over a median interval of 90 (IQR: 71-129) days among studies (62%) reporting assessment intervals. Declines were most pronounced during chemotherapy (± targeted therapy). INTERPRETATION: Declines in SMM are frequently observed during systemic cancer treatment, particularly during chemotherapy (± targeted therapy), although effect sizes were generally small per Cohen's thresholds. However, substantial heterogeneity limits interpretation of a single pooled estimate. Prospective studies with standardized methods are needed to clarify trajectories, mechanisms and clinical implications of SMM loss.