This observational study will investigate how immunotherapy affects physical fitness, quality of life, and treatment tolerance in adults with solid cancers. Immunotherapy can cause a range of side effects that impact daily functioning and may lead to treatment delays or early discontinuation. Physical fitness may influence how well patients cope with treatment, yet little is known about how fitness changes during immunotherapy or whether baseline fitness is linked to outcomes. Participants will complete fitness testing using cardiopulmonary exercise testing (CPET) and quality-of-life questionnaires before starting immunotherapy and again 12 weeks later. Blood samples will also be taken, and long-term outcomes including survival, disease progression, and quality of life will be followed for up to 24 months. All cancer treatment will remain standard of care. A small number of participants will be invited to take part in an optional research biopsy at week 12 to explore how physical fitness relates to changes in the tumour's immune environment. The study will help researchers understand natural changes in fitness during immunotherapy, identify whether baseline fitness is associated with treatment tolerance or outcomes, and generate information needed to design future trials testing exercise-based interventions during immunotherapy.
Physical fitness is a strong prognostic marker in cancer. Reduced cardiorespiratory fitness, measured objectively using cardiopulmonary exercise testing (CPET), is associated with higher perioperative risk, increased treatment-related complications, and poorer quality of life. Previous work from the study team and others has shown that chemotherapy and chemoradiotherapy for oesophageal and rectal cancer lead to significant declines in CPET-derived fitness, and that prescribed exercise prehabilitation can attenuate or reverse these declines and improve clinical outcomes. Immune checkpoint inhibitors have become standard of care for a growing range of solid tumours in both adjuvant and metastatic settings. Immunotherapy is associated with distinct patterns of toxicity, including immune-related adverse events and cumulative treatment-related side effects that can impair day-to-day functioning, result in treatment delays, or lead to early discontinuation. However, the impact of immunotherapy on objectively measured physical fitness, and the extent to which baseline fitness and changes in fitness relate to toxicity, quality of life, and long-term outcomes, remains poorly defined. Emerging evidence suggests complex interactions between physical fitness, immune function, and tumour biology. Exercise can influence systemic immunity and the tumour microenvironment, including increased infiltration of cytotoxic T cells and modulation of myeloid populations. These effects may help convert immunologically "cold" tumours with limited immune cell infiltration into "hot" tumours that are more responsive to immunotherapy. Understanding how baseline fitness and natural changes in fitness during immunotherapy relate to treatment tolerance and tumour-immune characteristics is therefore an important step towards rationally developing exercise-based interventions as potential adjuncts to immunotherapy. This Phase II window observational study is a prospective, single-centre cohort study with an embedded mechanistic sub-study. It will enrol adults with histologically confirmed solid malignancies who are starting standard-of-care immune checkpoint inhibitor therapy at University Hospital Southampton NHS Foundation Trust. The trial adopts a tumour-agnostic approach, stratifying participants by treatment setting (adjuvant vs metastatic/palliative) and immunotherapy regimen (single-agent vs dual-agent checkpoint inhibition). This reflects real-world practice and allows evaluation of how treatment context and intensity influence changes in fitness and attrition. For the observational cohort, participants will undergo baseline assessments within approximately two weeks prior to starting immunotherapy. These include CPET on a cycle ergometer to determine oxygen uptake at the anaerobic threshold (VO₂ at AT; primary outcome) and other CPET parameters, a panel of validated questionnaires assessing cancer-specific and generic quality of life, psychological distress, fatigue, social support and functional impact, grip strength, frailty assessment, targeted blood sampling (including nutritional markers, immune and metabolic biomarkers, and redox-related analytes), and review of standard-of-care imaging. Baseline medical history, comorbidities, and performance status will also be recorded. During the first 12 weeks of immunotherapy, all anti-cancer treatment will be delivered according to usual clinical practice, independent of study participation. The research team will prospectively collect data on immunotherapy regimens (drug, dose, schedule), immune-related and treatment-related adverse events graded using CTCAE v5.0 and Society for Immunotherapy of Cancer (SITC) criteria, treatment delays, dose modifications, permanent or temporary discontinuations, and health-care utilisation such as unplanned admissions. At approximately 12 weeks after immunotherapy initiation, participants will repeat the baseline battery of assessments: CPET, quality-of-life and psychosocial questionnaires, blood sampling, and documentation of treatment status. Radiological response will be evaluated using immune-adapted RECIST criteria on standard-of-care cross-sectional imaging where available. Participants will then enter long-term follow-up at approximately 6, 12, and 24 months from treatment start. Follow-up focuses on survival status, disease progression, ongoing treatment and toxicity, healthcare utilisation, repeated quality-of-life assessments, and selected clinical and nutritional measures. Questionnaires may be completed electronically, by telephone, or on paper, with a structured contact schedule to maximise response while respecting participant autonomy. An optional mechanistic sub-study will invite up to 10 participants to undergo a research tumour biopsy at around 12 weeks, in addition to use of surplus baseline diagnostic biopsy material where consent permits. Research biopsies will be obtained via image-guided percutaneous procedures or endoscopy, depending on tumour location and standard diagnostic pathways. Recruitment to the mechanistic component will be stratified by tumour immunogenicity (for example, tumours with higher versus lower mutational burden and immune infiltration) to facilitate comparison across immunologically "hot" and "cold" tumours. Tumour tissue will undergo multiplex immunohistochemistry and complementary molecular profiling to characterise the tumour and immune microenvironment, including quantification of key immune cell subsets (such as CD8⁺ T cells, CD4⁺ subsets, regulatory T cells, and myeloid populations), checkpoint marker expression, and spatial organisation. Parallel blood samples will be used to explore systemic redox biology, metabolic flexibility, and immune signatures. All samples will be pseudonymised and stored in a Human Tissue Authority-licensed tissue bank according to predefined governance procedures for up to ten years, to enable further ethically approved analyses. The observational component uses a precision-based sample size strategy. A total of 67 participants will be recruited across three strata, with 51 expected to contribute paired baseline and 12-week CPET data after accounting for differential attrition: adjuvant single-agent (20 recruited, 17 analysed), metastatic/palliative single-agent (23 recruited, 17 analysed), and metastatic/palliative dual-agent therapy (24 recruited, 17 analysed). This sample size allows estimation of mean change in VO₂ at AT with acceptable precision, with the overall 95% confidence interval spanning approximately ±0.55 standard deviations. Using planning values informed by prior exercise-oncology work (SD of change ≈1.8 mL/kg/min), 51 paired observations provide high power to detect a clinically important change of 1.5 mL/kg/min in VO₂ at AT, while recognising that the study is primarily exploratory and not powered for definitive hypothesis testing. The study will also estimate feasibility metrics such as recruitment, retention and completion of key assessments. The primary analysis will describe changes in CPET-derived fitness between baseline and 12 weeks of immunotherapy, using paired tests for within-participant change and stratified analyses by treatment setting and regimen. Secondary and exploratory analyses will examine changes in other CPET parameters, the incidence and pattern of immunotherapy-related toxicity and treatment discontinuation during the first 12 weeks, trajectories of quality-of-life and psychosocial outcomes, and longer-term survival and disease control up to 24 months. Associations between baseline fitness and subsequent toxicity, treatment modification, quality of life, and survival will be explored using appropriate regression and time-to-event methods. Mechanistic analyses will integrate tumour, blood, and clinical data using largely non-parametric and multivariable approaches to generate biologically plausible effect size estimates and hypotheses for future studies; these analyses are explicitly exploratory. Data will be collected in a secure, password-protected REDCap database with role-based access controls. CPET data will be processed according to standardised protocols, with key parameters independently reviewed by two exercise physiologists to support data quality. Routine data checks, range and consistency checks, and monitoring of recruitment and follow-up completeness will be undertaken by the trial team. Missing data will be described, and appropriate statistical methods for incomplete follow-up will be used where relevant; no complex imputation is planned for the primary outcome in this early-phase exploratory study. The study was developed with input from a patient and public involvement and engagement (PPIE) group comprising individuals with lived experience of cancer. They contributed to decisions on study burden and acceptability, including the timing and mode of assessments, communication around optional biopsies, and support for travel costs. Their feedback informed participant materials and recruitment strategies, and ongoing involvement is planned during study delivery and dissemination. Overall, this observational window study will characterise how immunotherapy affects objectively measured physical fitness and quality of life, clarify whether baseline fitness and early changes in fitness relate to toxicity and long-term outcomes, and provide mechanistic insight into links between fitness, immunotherapy, and the tumour microenvironment. These data are intended to define the natural history of fitness during immunotherapy, confirm that this represents a clinically meaningful problem, and provide the clinical and biological parameters needed to design a subsequent feasibility and effectiveness trial of structured exercise during immunotherapy.
Study Type
OBSERVATIONAL
Enrollment
67
This is an observational study with no study-assigned interventions. All participants receive standard-of-care immunotherapy as prescribed by their treating oncologist. Immunotherapy may include anti-PD-1, anti-PD-L1, anti-CTLA-4 agents, or approved combination regimens. All doses, schedules, treatment modifications, delays, and discontinuations follow routine clinical practice and manufacturer guidance. Treatment decisions are made independently of the study. The study observes and records treatment administration, effects on fitness and quality of life, adverse events, and clinical outcomes without influencing clinical care.
University Hospital Southampton NHS Foundation Trust
Southampton, Hampshire, United Kingdom
Change in Oxygen Uptake at Anaerobic Threshold (VO₂ at AT)
Change in oxygen uptake at the anaerobic threshold measured using cardiopulmonary exercise testing (CPET). VO₂ at AT will be reported in millilitres per kilogram per minute (mL·kg-¹·min-¹).
Time frame: Baseline and Week 12
Change in peak oxygen uptake (VO₂peak)
Change in peak oxygen uptake measured during CPET. Unit: mL·kg-¹·min-¹
Time frame: Baseline and Week 12
Change in peak power output
Peak power output measured during CPET, reported in watts (W).
Time frame: Baseline and 12 weeks
Change in ventilatory efficiency (VE/VCO₂ slope)
Ventilatory efficiency measured during CPET, reported as VE/VCO₂ slope (unitless ratio).
Time frame: Baseline and week 12
Cumulative Incidence of Immune-Related Adverse Events
Cumulative incidence of immunotherapy-related toxicity graded using Common Terminology Criteria for Adverse Events (CTCAE) v5.0 and Society for Immunotherapy of Cancer (SITC) immune-related adverse event criteria. Captured through systematic review during treatment phase. reported as CTCAE grade and/or proportion of participants with ≥Grade 3 toxicity (%).
Time frame: Baseline (start of immunotherapy) through Month 24
Treatment-Related Adverse Events Leading to Discontinuation
Proportion of participants discontinuing immunotherapy due to treatment-related toxicity, reported as a percentage of participants (%).
Time frame: Baseline through Month 24
Change in cancer-specific quality of life
Cancer-specific quality of life assessed using the European Organisation for Research and Treatment of Cancer Quality of Life Questionnaire - Core 30 (EORTC QLQ-C30) Global Health Status/QoL score. Unit of Measure: Score on a scale (0-100). Scale Details: 0 = worst quality of life, 100 = best quality of life. Higher scores indicate better quality of life.
Time frame: Baseline, Week 12, Month 6, Month 12, and Month 24
Change in general health status
General health status assessed using the EuroQol 5-Dimension 5-Level questionnaire (EQ-5D-5L) index score. Unit of Measure: Index score. Scale Details: Index values typically range from \<0 (health states worse than death) to 1 (perfect health) Higher scores indicate better health status
Time frame: Baseline, Week 12, Month 6, Month 12, and Month 24
Change in psychological distress
Psychological distress assessed using the National Comprehensive Cancer Network (NCCN) Distress Thermometer. Unit of Measure: Score on a numeric rating scale (0-10) Scale Details: 0 = no distress 10 = extreme distress Higher scores indicate worse distress
Time frame: Baseline, Week 12, Month 6, Month 12, and Month 24
Change in anxiety and depression symptoms
Anxiety and depression symptoms assessed using the Patient Health Questionnaire-4 (PHQ-4). Unit of Measure: Total score Scale Details: Range 0-12 Higher scores indicate greater anxiety and depressive symptoms
Time frame: Baseline, Week 12, Month 6, Month 12, and Month 24
Change in fatigue severity
Fatigue severity assessed using the Patient-Reported Outcomes Measurement Information System (PROMIS) Fatigue Short Form: reported as T-score (mean 50), higher scores indicate worse fatigue.
Time frame: Baseline, Week 12, Month 6, Month 12, and Month 24
Change in perceived social support
Modified Medical Outcomes Study Social Support Survey (mMOS-SSS); score range 0-100, higher scores indicate greater support.
Time frame: Baseline, Week 12, Month 6, Month 12, and Month 24
Change in functional impairment
Work and Social Adjustment Scale (WSAS); total score range 0-40, higher scores indicate worse impairment.
Time frame: Baseline, Week 12, Month 6, Month 12, Month 24
Change in functional capacity
Duke Activity Status Index (DASI); score range 0-58.2, higher scores indicate better functional capacity
Time frame: Baseline, Week 12, Month 6, Month 12, Month 24
Change in frailty status
Edmonton Frail Scale (EFS); total score range 0-17, higher scores indicate worse frailty.
Time frame: Baseline, Week 12, Month 6, Month 12, Month 24
Recruitment feasibility
Proportion of eligible participants who consent to the observational study, calculated as number consented divided by number screened, reported as percentage (%).
Time frame: During recruitment period - 12 months
Adherence to research assessments
Proportion of participants completing each scheduled research assessment (e.g. CPET, questionnaires), reported as percentage (%).
Time frame: Baseline and Week 12
Feasibility of Optional Research Biopsy
Proportion of participants who consent to and complete the optional Week-12 research biopsy, reported as a percentage (%).
Time frame: Week 12
Biopsy-related complications
Proportion of participants experiencing biopsy-related complications following the optional Week-12 research biopsy, reported as a percentage (%).
Time frame: Week 12
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