A randomized clinical study on the impact of Comprehensive Geriatric Assessment (CGA) based interventions on the quality of life of elderly, frail, onco-hematologic patients candidate to anticancer therapy: protocol of the ONCO-Aging study

The ONCO-Aging study is a prospective, randomized study and includes a clinical trial and a collateral biologic study. Patients older than 65 years, with hematological or oncological neoplasms, who refer for treatment to the Oncology, Hematology and Radiation Oncology Divisions of the University Hospital Maggiore della Carità in Novara, IT, and candidate to therapies with innovative target directed agents or to combined schedules including RT and CT, are screened for frailty by the G8 questionnaire; according to previous evidence, a score ≤ 14/17 is considered the threshold for frailty [16, 17]. Targeted directed agents include the following drugs: tyrosine-kinase inhibitors (TKis), monoclonal antibodies and immune checkpoint inhibitors (ICIs), alone or in combination schedules with CT. Combined treatment schedules including RT and CT are also included. Patients with a G8 score ≤ 14/17, are randomized in a 1:1 ratio to the following procedures: arm A, onco-geriatric evaluation by CGA; arm B, standard clinical care, according to local practice. Figure 1 shows the flowchart of the study. Patients are randomized by a REDCap dedicated system. Patients assigned to arm A undergo a CGA at baseline, before treatment start and every 6 months thereafter and may receive a CGA based geriatric intervention if required according to the geriatrician judgement (Fig. 2). Patients in arm B are managed according to clinical practice (Fig. 3). Blood samples to assess the prognostic and predictive value of cell-derived data (MDSC and T cell senescence) and their modification with treatment, will be collected at baseline and at the time of disease progression. Blood samples from healthy, age-matched controls, are recruited on a voluntary basis and also from the UPO Biobank.

The aim of the biological study is to assess the presence and the modifications induced by treatments of senescent T cell and MDSC in the peripheral blood of enrolled patients in both arms to evaluate the correlation with treatment efficacy and patient characteristics, including comorbidities, concomitant drugs, and lifestyle habits.

The primary endpoint is Health Related Quality of Life, based on the EORTC QLQ C30 questionnaire [18]; EORTC QLQ C30 questionnaire will be administered at baseline and every 3 months during treatment/follow up.

The sample size was estimated by a two-tailed t-test (alpha = 0. 05, power = 0. 8 and an effect size Cohen (ES) equal to 0. 5) for a minimum clinically relevant difference of 10 points (SD = 20) on the global EORTC QLQ C30 Quality of Life scale. The planned sample size is 144 patients (72 per arm), considering a 10 % loss at follow-up. The primary endpoint will be evaluated on the ITT population. Baseline data will be summarized in terms of mean, standard deviation, median, I and III quartile, for continuous variables, and percentages for categorical variables. A test for the difference between two queued averages will be applied when comparing the total score for QoL. A level of significance of 5 % will be considered statistically significant. The study is expected to enroll about 144 patients with solid tumor neoplasms or hematological malignancies candidate to a first line treatment for advanced disease.

The ONCO-aging study was approved by the referral Ethical Committee (EC) of Maggiore della Carità Hospital, in Novara, IT, on December 18, 2019 (CE 230/19). Accrual in the ONCO-AGING trial started on January 14, 2020; study is actively recruiting. Main inclusion criteria are: age ≥ 65 years; diagnosis of advanced solid tumor or hematologic cancer at any stage, candidate to first line therapy with innovative target agents or combined RT and CT schedules; G8 score ≤ 14/17; signed IC. Patients with a life expectancy < 3 months are excluded.

Comprehensive Geriatric Assessment (CGA): in arm A, patients receive a dedicated geriatric examination (60–90 min), administered by a dedicated geriatrician, and are classified according to CGA results and the Rockwood Frailty Index (RFI) as “frail” (RFI > 0.25), “unfit/prefrail” (0.08 > RFI < 0.25) or “fit” (< 0.08) [19].

The CGA includes evaluation of cognitive status with the Mini Mental State Examination (MMSE), Clock drawing test (CDT), and Montreal Cognitive Assessment (MOCA) [20]; of psychosocial status by the means of Geriatric Depression Scale (GDS) and Social Vulnerability Index (SVI) [21]; of disability by Activities of Daily Living (ADL) and Instrumental Activities of Daily Living (IADL) [22, 23]; of nutritional status by Mini Nutritional Assessment (MNA) [24]; of comorbidities by Cumulative Illness Rating Scale for Geriatrics (CIRS-G) and of pharmacological impact by number of drugs [25]; of sarcopenia and physical performance by Hand Grip Strength, Timed Up and Go test, Tinetti Scale, and number of falls in last six months [26]. CGA is performed at baseline and every 6 months. If issues are found in the areas of fragility, mid-term evaluations are foreseen, as indicated by the geriatrician. CGA based interventions will cover nutritional imbalance, social issues including the availability of caregiver and psychological interventions by dedicated psyco-oncologists.

In both arms, QoL assessment by the standardized EORTC QLQ-C30 questionnaire is performed at baseline (before treatment start) and every 3 months. Disease evaluation is performed in both arms according to local clinical practice. Patients are observed for up to 12 months or until disease progression (Fig. 4).

The study is designed to evaluate T senescent cells and MDSC, and their modifications with treatment, in the peripheral blood of patients enrolled in the ONCO-aging study; blood samples will be collected at baseline (before start of therapy) and at the time of disease progression.

Blood samples (10 ml whole blood in Vacutainer EDTA tubes) are processed and analysed at the Immuno-Oncology Laboratory, at the Center for Translational Research on Autoimmune & Allergic Diseases – UPO-CAAD, in Novara, IT.

Peripheral mononuclear blood cells (PBMCs) are collected and isolated by Ficoll/Hypaque density gradient. T CD3 + Lymphocytes are isolated from the PBMCs by magnetic beads. The following markers will be tested by reverse transcription quantitative PCR, according to a manufactory protocol: p16INK4a and p21Cip/Waf1.

The Enzyme-Linked ImmunoSorbent Assay (ELISA) is used to evaluate the expression of cytokines and chemokines (e.g. CCL2/MCP-1, IFNγ, IL-6, IL-8), in plasma obtained from the same blood samples.

MDSC analysis is performed by flow cytometry in PBMCs. Assessment of MDSC phenotype is characterised by using the following markers: for monocytes-MDSC CD14⁺HLA-DR⁺, and for granulocytes-MDSC CD15⁺CD33^int and LOX-1⁺. Biological markers for T cell senescence and MDSC characterization are detailed in Table 1.