Abstract
The number of older patients with cancer is increasing as a result of the ageing of Western societies. Immune checkpoint inhibitors have improved cancer treatment and are associated with lower rates of treatment-related toxicity compared with chemotherapy in the general population. Nonetheless, immune checkpoint inhibitors have potentially serious immune-related adverse events, which might have a greater impact on older and more vulnerable patients and potentially influence treatment efficacy and quality of life. Previous clinical trials have shown no major increase in immune-related adverse events; however, older patients are underrepresented and relatively healthy in these trials. Observational studies suggest that older and more vulnerable patients may be at a higher risk of immune-related adverse events and early treatment discontinuation. Geriatric assessment could help identify older patients who will benefit from immune checkpoint inhibitors.
Key Points
| Previous clinical trials did not show major increases in immune-related adverse events in older patients. |
| Limited available observational studies suggest that older and more vulnerable patients may be at a higher risk of immune-related adverse events and early treatment discontinuation. |
| Geriatric assessment could help identify older patients that will benefit from immune checkpoint inhibitors. |
Introduction
In recent years, the number of older patients with cancer is strongly increasing as a result of the ageing of Western societies. In the Netherlands, 45% of patients with melanoma, 68% of patients with lung cancer and 69% of patients with urinary tract cancer are aged older than 65 years [1]. Cancer in older patients frequently appears in the context of comorbid diseases, frailty and geriatric problems such as physical or cognitive impairment [2], which has been shown to affect the ability to endure toxic cancer treatments [3]. Previous studies demonstrated that older patients are at increased risk of chemotherapy toxicity [3]. Additionally, the risk of dying from other causes increases with age [4, 5], which means that some patients may not have the remaining life expectancy to benefit from anti-cancer therapy. Therefore, it is important to weigh the benefits and risks of anti-cancer treatment in older patients.
In recent years, immunotherapy targeting checkpoint inhibition has improved the treatment of different types of cancer. Immunological checkpoint molecules suppress the attack of tumour-specific T cells, which usually are an integral part of anti-tumour immunity [6, 7]. Some checkpoint inhibitors block the interaction between programmed cell death-1 (PD-1) on T cells and its ligand PD-L1 on cancer cells and myeloid cells [6, 8]. Others target cytotoxic T-lymphocyte antigen-4 (CTLA-4), which blocks negative signals during T-cell interaction with antigen-presenting cells and depletes regulatory T cells, thereby restoring and enhancing T-cell reactivity [9, 10]. These drugs are used in an expanding group of tumour types but are most successful in advanced and metastasized melanoma, where progression-free survival (PFS) and overall survival (OS) have strongly improved [11–14].
However, it is possible that checkpoint inhibitors may be less efficient in older patients because of an ageing immune system (immunosenescence) [6, 7]. The numbers of dendritic cells and CD4+ naive T cells decline while the pool of terminally differentiated CD8+ T cells increases [7, 15]. In addition, the number of circulating and intra-tumoural myeloid-derived suppressor cells increases. Hence, T-cell function may decrease and lead to impaired responsiveness to therapies aiming to boost tumour immunity [6, 16]. Treatment with checkpoint inhibitors is expensive, costing around 50,000–80,000 euros per treatment [17]. Because checkpoint inhibitors potentially have serious adverse events and are costly, it is essential to determine which patients truly benefit from therapy and at what risk. The aim of this review is to provide a summary of available efficacy data, to provide an overview of the occurrence of adverse events of checkpoint inhibitors in older patients and to evaluate the available evidence on the treatment of these adverse events. We performed an explorative search on PubMed using the following keywords: “Elderly”, “Older”, “Immune Checkpoint Inhibitors”, “Immunotherapy”, “Toxicity”, and “Immune-related adverse events”. We additionally searched through the references of the publications found and we searched abstracts presented at recent oncology conferences.
Treatment Efficacy of Immune Checkpoint Inhibitors in Older Patients
Melanoma
Several studies have shown the effectiveness of immune checkpoint inhibitors in melanoma for patients of all ages. In 2018, an update of the Cochrane review was performed with respect to systemic treatments for metastatic cutaneous melanoma [18], which showed that with regard to immune checkpoint inhibitors, anti-PD-1 improved OS compared with chemotherapy, and probably improved PFS. Anti-PD-1 was associated with a better OS and PFS compared with anti-CTLA-4. Anti-CTLA-4 plus chemotherapy probably increased PFS compared with chemotherapy alone, but was not significantly associated with an OS gain. Last, the combination of anti-CTLA-4 plus anti-PD-1, as compared with anti-CTLA-4 alone, was associated with better PFS. Patients in this Cochrane review had a mean age of 57.5 years at the time of treatment randomisation, representing a younger population than general patients with melanoma (Table 1).
Table 1.
Overview of systemic treatments for metastatic cutaneous melanoma [18]
| Cochrane review | Relative effect (95% CI) | No. of patients (studies) | Quality evidence (grade) |
|---|---|---|---|
| Anti-PD-1 compared with chemotherapy | |||
| Overall survival | HR 0.42 (0.37–0.48) | 418 (1) | High |
| Progression-free survival | HR 0.49 (0.39–0.61) | 957 (2) | Moderate |
| Tumour response | RR 3.42 (2.38–4.92) | 1367 (3) | High |
| Toxicity (≥ G3) | RR 0.55 (0.31–0.97) | 1360 (9) | Low |
| Anti-PD-1 compared with anti-CTLA-4 | |||
| Overall survival | HR 0.63 (0.60–0.66) | 764 (1) | High |
| Progression-free survival | HR 0.54 (0.50–0.60) | 1465 (2) | High |
| Tumour response | RR 2.47 (2.01–3.04) | 1465 (2) | High |
| Toxicity (≥ G3) | RR 0.70 (0.54–0.91) | 1465 (2) | Low |
| Anti-CTLA-4 + chemotherapy compared with chemotherapy | |||
| Overall survival | HR 0.81 (0.65–1.01) | 1157 (2) | Low |
| Progression-free survival | HR 0.76 (0.69–0.92) | 502 (1) | Moderate |
| Tumour response | RR 1.28 (0.92–1.77) | 1157 (2) | Moderate |
| Toxicity (≥ G3) | RR 1.69 (1.19–2.42) | 1142 (2) | Moderate |
| Anti-CTLA-4 + anti-PD-1 compared with anti-CTLA-4 (overall survival not measured) | |||
| Progression-free survival | HR 0.40 (0.35–0.46) | 738 (2) | High |
| Tumour response | RR 3.50 (2.07–5.92) | 738 (2) | High |
| Toxicity (≥ G3) | RR 1.57 (0.85–2.92) | 764 (2) | Low |
CI confidence interval, CTLA-4 cytotoxic T-lymphocyte antigen-4, G3 grade 3, HR hazard ratio, PD-1 programmed cell death-1, RR relative risk
In the general older patient population, evidence with regard to the efficacy and toxicity of CTLA-4 inhibitors is lacking. A meta-analysis including patients with melanoma, lung and renal cell cancer suggested that older patients benefit from anti-CTLA-4 therapy in terms of OS with a hazard ratio (HR) of 0.73 [95% confidence interval (CI) 0.62–0.87; p < 0.001] in comparison with the control regimen [8]. For anti-PD-1 treatment, a retrospective study by Betof et al. showed no difference in OS or PFS in patients with metastatic melanoma, comparing patients aged ≥ 75 years with younger patients [19]. However, only 20–40% of patients included in these trials are aged > 65 years[20], while 45% of the general melanoma population is aged > 65 years [1]. The older patients included in these trials are probably not representative for the general population of patients with cancer because of selective inclusion criteria, such as a good performance status, normal hepatic and renal function, and no autoimmune disease. Furthermore, studies have shown that older patients discontinue their treatment more often than younger patients, possibly decreasing effectiveness [21].
Non-Small Cell Lung Cancer
Khan et al. performed a meta-analysis of the available evidence from randomised controlled trials in 2018 comparing anti-PD-1 or PD-L1 therapies and chemotherapy in the treatment of advanced non-small cell lung cancer (NSCLC) [22]. A total of seven randomised controlled trials were selected for inclusion; anti-PD-1 or PD-L1 therapies resulted in a better OS, PFS, and objective response rate in comparison to chemotherapy with pooled HRs of 0.72 (95% CI 0.63–0.82; p < 0.00001), 0.84 (95% CI 0.72–0.97; p < 0.02) and odds ratio 1.52 (95% CI 1.08–2.14; p < 0.02), respectively. In subgroup analyses for OS, a significant HR was found in patients aged above 65 years [HR 0.71 (95% CI 0.56–0.91; p = 0.006)]; however, there was no benefit for patients above 75 years [HR 1.23 (95% CI 0.61–2.48; p = 0.56)]. For PFS, no significant association was found in subgroup analyses, with an HR of 0.78 (95% CI 0.57–1.09; p = 0.14 for patients over the age of 65 years and 1.25 (95% CI 0.70–2.22; p = 0.45) for patients over the age of 75 years, respectively. A systematic review and meta-analysis by Peng et al. showed that immune checkpoint inhibitor combination therapy was significantly associated with prolonged OS in NSCLC [HR 0.80 (95% CI 0.73–0.88; p < 0.00001)], but not in SCLC [HR 0.94 (95% CI 0.82–1.08; p = 0.40)]. Furthermore, the data suggested a higher efficacy for PD-1 inhibitors than PD-L1 or CTLA-4 inhibitors; however, no specific data for older patients were reported [23].
Bladder and Renal Cell Cancer
The first breakthrough in cancer therapy for metastatic bladder cancer was in 2016 with the approval of atezolizumab for patients who have disease progression during or following chemotherapy, or have disease progression within 12 months of (neo)adjuvant treatment with chemotherapy [24]. Since then, four additional checkpoint inhibitors have been approved [25]: durvalumab and avelumab (PD-L1 blockade) as well as nivolumab and pembrolizumab (PD-1 blockade). From the five available inhibitors, pembrolizumab is the only drug with level I evidence from a phase III trial specifically in urothelial cancer. An improved OS was seen in the KEYNOTE-045 study [26] with a median OS of 10.3 months as compared with 7.4 months in the chemotherapy arm. There are several ongoing trials in patients with urothelial cancer with immune checkpoint inhibitors; however, specific data for older patients are not yet available [27].
A recent meta-analysis with respect to metastatic renal cell cancer showed an improved survival with an HR of 0.75 (95% CI 0.66–0.85; p < 0.001) for immunotherapy as first- or second-line therapy compared with standard of care and an improved PFS with an HR of 0.88 (95% CI 0.80–0.97; p = 0.009) [28]. Unfortunately, no specific data for older patients were presented and those included in the trials are usually not representative of the general older population.
Immune-Related Adverse Events in Older Patients
It was shown that chemotherapy toxicity occurs more frequently in older patients than younger patients [3]. We hypothesise that, because of an ageing immune system, age-related comorbidity and decreased functional reserve, older patients might also experience more immune-related toxicities with greater impact owing to hospitalisation. Immune checkpoint inhibitors are responsible for specific inflammatory toxicities by increasing the activity of the immune system. These adverse events are referred to as immune-related adverse events (irAEs). The precise underlying mechanism is unknown. Translational studies in patients with irAEs have shown that T-cell response, antibodies and cytokine responses may all be involved [29]. The majority of irAEs occur within the first 4 months of treatment, but these events can occur at any time during treatment or several months after discontinuation [29, 30].
Nearly all organs can be affected: the skin, gastrointestinal tract, endocrine glands, lung, nervous system, liver, kidney, hematological cells, musculo-articular system, heart and eyes. The spectrum of toxicities seen in CTLA-4 inhibitors or PD-1/PD-L1 inhibitors is similar, but frequencies differ. In general, CTLA-4 inhibitors have shown more grade 3–4 irAEs than PD-1/PD-L1 inhibitors [20, 30]. In addition, the combination of anti-CTLA-4 and PD-1/PD-L1 blockade for metastatic melanoma can cause treatment-related adverse events in 95% of patients, with grade 3 or higher events in 55% of patients [31].
With regard to toxicity in older patients, previous randomised trials have rarely studied these outcomes in relation to age. Most evidence is derived from subgroup analyses and cross trial meta-analyses of larger clinical trials. Table 2 summarises the data from trial subgroup analyses, when published.
Table 2.
Overview of trial data regarding immune-related adverse events (irAEs) in elderly patients with cancer
| Study (first author, year) | No. of patients | Tumour type | Checkpoint inhibitor | Relevant outcome | Results |
|---|---|---|---|---|---|
| Friedman, 2016 [21] |
Patients aged ≥ 80 years N = 98 |
Melanoma |
Ipilimumab Nivolumab Pembrolizumab Combination ipilimumab + nivolumab |
irAEs |
Any grade irAEs Ipilimumab (n = 74): 87.8% Anti-PD-1 (n = 24): 87.5% Nivolumab + ipilimumab (n = 8): 87.5% Grade 3 or 4 irAEs Ipilimumab (n = 74): 29.7% Anti-PD-1 (n = 24): 20.8% Nivolumab + ipilimumab (n = 8) 62.5% |
| Nosaki, 2019 [35] |
Patients aged ≥ 75 years Pooled analysis Pembrolizumab N = 149 Chemo N = 105 |
NSCLC | Pembrolizumab | irAEs |
Any treatment-related AE Pembrolizumab: age ≥ 75 years: 68%, age < 75 years: 65% Chemo: age ≥ 75 years: 94%, age < 75 years: 87% Grade 3–5 treatment-related AE Pembrolizumab: age ≥ 75 years: 24%, age < 75 years: 17% Chemo: age ≥ 75 years: 61%, age < 75 years: 39% irAEs and infusion reactions Pembrolizumab: age ≥ 75 years: 25%, age < 75 years: 25% Chemo: age ≥ 75 years: 7%, age < 75 years: 6% |
| Spigel, 2017 [37] |
N = 1308 520 aged ≥ 70 years ECOG PS 2 N = 108 |
NSCLC | Nivolumab | TRAEs |
Any grade TRAE Age ≥ 70 years: 62%, age < 70 years: 59% ECOG PS 2: 46%, ECOG PS 0–1: 61% Grade 3–4 TRAE Age ≥ 70 years: 12%, age < 70 years: 11% ECOG PS 2: 10%, ECOG PS 0–1: 12% Grade 5 TRAE Age ≥ 70 years: < 1%, age < 70 years: < 1% ECOG PS 2: 2%, ECOG PS 0–1: < 1% |
| Herin, 2018 [39] |
N = 220 46 aged ≥ 70 years |
Bladder carcinoma NSCLC Gastrointestinal cancer Gynaecological cancer Head and neck carcinoma Breast cancer Renal cell carcinoma |
Anti-PD-1/PD-L1 monotherapy Anti-PD-1/PD-L1 + other immuno- modulatory monoclonal antibodies Anti-PD-1 + targeted therapy |
irAEs |
Grade 1 irAE Age ≥ 70 years: 72% Age < 70 years: 48% Grade 2 irAE Age ≥ 70 years: 41% Age < 70 years: 20% Grade 3–4 irAE Age ≥ 70 years: 22% Age < 70 years: 13% Median time before first event Age ≥ 70 years: 16d Age < 70 years: 36d |
AE adverse event, Chemo chemotherapy, d days, ECOG PS ECOG performance status, Ipi ipilimumab, N number of included patients, Nivo nivolumab, NSCLC non-small cell lung cancer, PD-1 programmed cell death-1, PD-L1 programmed cell death-ligand 1, TRAE treatment-related adverse event
Cytotoxic T-Lymphocyte Antigen-4 Inhibitors: Trial Data
Previous studies have reported irAEs in 60–86% of patients of all ages using ipilimumab (CTLA-4 inhibitor). Around 20–41.6% of patients develop grade 3 and 4 toxicities, depending on dose [20, 30, 32]. The most frequently observed toxicities (> 10%) are diarrhea, rash, pruritus, fatigue, nausea, vomiting, anorexia and abdominal pain [20, 30].
Friedman et al. reported a toxicity analysis of published phase III data in a small group of patients aged older than 80 years treated with different immune checkpoint inhibitors for melanoma. The rate of irAEs and early treatment discontinuation was modestly higher in older patients compared with a younger population. This effect was especially seen in combination therapy [7, 21].
Programmed Cell Death-1/Programmed Death-Ligand 1 Inhibitors: Trial Data
For nivolumab, 58–85% of patients of all ages reported irAEs, of which 7–20% were grade 3 and 4 toxicities, depending on tumour localisation. For pembrolizumab, 57–80% of patients reported irAEs, of which 10–26% were grade 3 and 4 toxicities, depending on dose [20, 30, 32]. The most commonly observed toxicities (> 10%) are fatigue, rash, pruritus, diarrhoea, nausea and arthralgia [20, 30].
The KEYNOTE trials have investigated the efficacy of pembrolizumab in 3991 patients with melanoma, NSCLC, head and neck cancers, urothelial carcinoma and Hodgkin’s lymphoma. Forty-six percent of the patients were age ≥ 65 years and 16% were age ≥ 75 years. No overall differences in safety were observed between older and younger patients [33, 34]. This was recently confirmed in an update that was presented at the European Lung Cancer Congress 2019, in which it was shown that there was no difference in irAEs between patients aged < 75 and > 75 years [35].
The Checkmate trials assessed treatment with nivolumab for NSCLC, melanoma and renal carcinoma. In total, 1359 patients were treated with nivolumab, of whom 39% were aged ≥ 65 years and 9% were aged ≥ 75 years. No overall differences in safety were observed between older and younger patients [33, 36]. Spigel et al. presented a pooled analysis of 520 patients aged ≥ 70 years and 108 patients with a baseline Eastern Cooperative Oncology Group (ECOG) performance status of 2, receiving nivolumab for metastatic NSCLC in the Checkmate 153 trial. There was no difference in the incidence of treatment-related adverse events, any grade and grade 3–5, between the older and younger patients and between the patients with ECOG performance status 2 and 0–1 [37].
The US Food and Drug Administration published a subset analysis of the safety of nivolumab in elderly patients. They reviewed 1030 patients in registration trials of lung cancer, renal cancer and melanoma. The data show more reported grade 3–5 adverse events in patients aged ≥ 70 years and a trend towards a higher incidence of irAEs requiring treatment with immune-modulating medication in this group. The indications for immune-modulating medication were mostly rash or colitis [33, 38].
Herin et al. analysed patients with advanced solid tumours enrolled in 14 immunotherapy phase I/II trials, comparing all included patients aged ≥ 70 years with patients aged < 70 years. Median age in the older patient group was 75 years with an ECOG performance status 0–1. Cumulative incidence of grade 1–2 irAEs was significantly higher in older patients compared with younger patients. The data show a trend towards a higher incidence of grade 3–4 irAEs, occurring in 22% of older patients vs. 13% in younger patients. However, the difference was not statistically significant. Median time before the occurrence of a first event was shorter in older patients [39].
The clinical immunotherapy trials included only 20–40% of patients aged > 65 years [20]. Therefore, it must be noted that the data are derived from trials including primarily patients below the age of 75 years and with an ECOG performance status of 0–1 or Karnofsky performance status of 80–100, while the general population of older patients with cancer is generally older and has a lower performance status [9, 14, 31, 32, 40–43]. It is conceivable that more vulnerable older patients with a decreased functional reserve experience more adverse events with a greater impact on quality of life.
Population-Based Data
There have been some previous observational studies in older patients who received immunotherapy that included a population-based sample of older patients, which is more likely to resemble daily clinical practice. Table 3 summarises these studies. For example, Sattar et al. performed a retrospective study on the efficacy and toxicity of ipilimumab, pembrolizumab, and nivolumab including 23 patients aged ≥ 75 years with a median Charlson comorbidity score of 6.8. They found no statistically significant differences in irAEs, severity of grade 3 or higher, multiple irAEs, need for corticosteroid treatment and types of adverse events when comparing different age groups. However, the data showed a trend to more irAEs of any severity and irAEs grade ≥ 3 occurring in the age ≥ 75 years group. The most frequently reported irAEs were skin toxicity, gastrointestinal toxicity and endocrinopathy [44].
Table 3.
Overview of observational studies regarding immune-related adverse events in elderly patients with cancer
| Study (first author, year) | No. of patients | Tumour type | Checkpoint inhibitor | Relevant outcome | Results |
|---|---|---|---|---|---|
| Sattar, 2018 [44] |
N = 78 26 (33%) aged 65–74 years, 23 (30%) aged ≥ 75 years |
Melanoma NSCLC Renal cell carcinoma |
Ipilimumab Nivolumab Pembrolizumab |
irAEs |
41 (53%) patients with irAEs, 12 (15%) multiple irAEs Any grade irAEs Age < 65 years (n = 29): 41% Age 65–74 years (n = 26): 58% Age ≥ 75 years (n = 23): 61% Grade ≥ 3 irAEs Age < 65 years (n = 17): 29% Age 65–74 years (n = 12): 25% Age ≥ 75 years (n = 11): 36% |
| Chiarion Sileni, 2014 [45] | N = 855, 193 patients aged > 70 years | Melanoma | Ipilimumab | irAEs |
Any irAE: age > 70 years: 50%, age < 70 years 46% Grade 3–4 irAE: age > 70 years: 6%, age < 70 years: no data |
| Leroy, 2019 [46] | N = 52, 23 patients aged ≥ 80 years | Melanoma | Ipilimumab |
irAEs Treatment irAEs Hospitalisation because of irAEs |
Any irAE: age ≥ 80 years: 65%, age ≤ 80 years: 52% Grade ≥ 3 irAE: age ≥ 80 years: 22%, age ≤ 80 years: 19% Corticosteroid treatment: age ≥ 80 years: 22%, age ≤ 80 years: 19% Additive immunosuppressive therapy: age ≥ 80 years: 9%, age ≤ 80 years: 4% Hospitalisation: age ≥ 80 years: 22%, age ≤ 80 years: 9% |
| Freeman, 2015 [47] | N = 148, 52 (35%) aged ≥ 65 years | Melanoma | Nivolumab | irAEs |
Most common irAEs: Rash: Age ≥ 65 years: 40.4%, age < 65 years: 38.5% Diarrhoea: age ≥ 65 years: 21.2%, age < 65 years: 30.2% Vitiligo: age ≥ 65 years: 7.7%, age < 65 years: 10.4% |
| Betof, 2017 [19] | N = 254, 65 (25.6%) aged 65–74 years, 47 (18.5%) aged ≥ 75 years | Melanoma |
Anti-PD-1 Anti-PD-L1 |
irAEs |
110 (43.3%) irAEs in all patients Age 65–74 years: more arthritis (10.8%, p = 0.02) Age ≥ 75 years trend to more endocrine toxicity |
| Wong, 2017 [48] | N = 91, 64% ECOG PS 0–1, 18% ECOG PS 2, 9% ECOG PS 3 | Melanoma | Anti-PD-1 | irAEs |
Treatment-related AEs grade ≥ 3: ECOG PS 0–1: 5% ECOG PS 2: 13% ECOG PS: 30% irAEs grade ≥ 3: ECOG PS 0–1: 15% ECOG PS 2: 0% ECOG PS 3: 0% |
| Horvat, 2015 [49] | N = 298 | Melanoma | Ipilimumab |
Number of irAEs Treatment irAEs |
254 (85%) irAE 56 (19%) treatment discontinuation 103 (35%) corticosteroid treatment 29 (10%) anti-TNFα treatment |
| Luciani, 2018 [50] |
Patients aged ≥ 75 years N = 72 |
NSCLC |
Nivolumab Pembrolizumab |
irAEs |
9 (14%) irAEs 4 (40%) grade 3–4 irAEs |
| Corral de la Fuente, 2019 [51] |
N = 98 27 aged ≥ 70 years |
NSCLC |
Anti-PD-1 Anti-PD-L1 |
irAEs |
30.6% irAEs No statistically significant differences between older and younger patients |
| Verzoni, 2019 [52] |
N = 389 70 aged ≥ 75 years |
Renal cell carcinoma | Nivolumab |
drAEs irAEs Treatment discontinuation |
32% any drAE 7% grade ≥ 3 drAE 20% any grade irAE 2% grade 3 irAE <1% grade 4 irAE 7.9% treatment discontinuation, of which 45% because of irAEs |
| Muchnik, 2019 [53] |
Patients aged ≥ 70 years N = 75 53% CCI ≥ 3 49% ECOG PS ≥ 2 |
NSCLC |
Nivolumab Pembrolizumab “Other” |
irAEs Treatment irAEs Hospitalisation |
37% of any grade irAE 8% grade ≥ 3 irAE 64 patients discontinued treatment, 15% because of irAEs 64% of patients with irAE glucocorticoid treatment 72% hospitalisation during treatment |
| Silva, 2018 [54] |
Patients aged ≥ 65 years N = 106 |
Lung cancer Melanoma Urological cancer Colorectal cancer |
Nivolumab Pembrolizumab Ipilimumab Atezolizumab |
irAEs |
21 irAEs 5 severe irAEs Frailty predicted risk to AE: OR 3.03 (95% CI 1.36–6.74; p = 0.006) |
AE adverse event, CCI Charlson Comorbidity Index, CI confidence interval, drAE drug-related adverse event, ECOG PS ECOG performance status, irAEs immune-related adverse events, N number of included patients, NSCLC non-small cell lung cancer, OR odds ratio, PD-1 programmed cell death-1, PD-L1 programmed cell death-ligand 1, TNF tumour necrosis factor
Chiarion Sileni et al. reported that patients with melanoma aged over 70 years using ipilimumab had similar rates of adverse events compared to patients aged ≤ 70 years, 50% vs. 46% of any grade and 6% grade 3–4. The most frequently reported irAEs in patients aged over 70 years were pruritus, rash, diarrhea, nausea and liver toxicity. The median age in patients aged > 70 years was 75 years, but with an ECOG performance status of 0 or 1 in 97% of the patients [45], which was not a representative population in daily practice.
Leroy et al. analysed a retrospective cohort of patients aged over 80 years treated with ipilimumab for melanoma. Only 23 elderly patients were included, with a median age of 82 years. They had Charlson comorbidities scores of 0–3 and 96% of the patients had an ECOG performance status 0–1. In this study, 65% of elderly patients reported adverse events, with 22% grade 3 and there was one grade 5 adverse event. Of these patients, 22% of patients needed corticosteroid treatment, two patients needed additive immunosuppressive therapy, four were hospitalised and three had to discontinue ipilimumab. The grade 3 adverse events reported were hepatitis, colitis, hypophysitis and pneumopathy. The authors concluded that irAEs occur at the same rate in older patients compared to younger patients in this study and compared to previously reported studies [46].
Freeman et al. performed a retrospective analysis of irAEs in a cohort of melanoma patients aged < 65 years compared to patients aged > 65 years treated with nivolumab. This analysis showed no significant difference in the incidence of irAEs or the irAE profile between the two age groups. The most commonly reported irAEs were diarrhoea/colitis, rash and vitiligo. However, no data on the ECOG performance status and severity of irAEs were provided [47].
In addition, Betof et al. retrospectively analysed 254 patients receiving anti-PD-1 and/or PD-L1 for metastatic melanoma, including 65 patients aged 65–74 years and 47 patients aged ≥ 75 years. The incidence of arthritis was significantly higher among patients aged 65–74 years. Patients aged ≥ 75 years had a higher incidence of thyroiditis or endrocrine-related toxicity; however, this was not statistically significant. No significant differences in dermatitis, colitis, hepatitis or pneumonitis were reported between the different age groups. The grade of severity of the adverse events was not reported [19].
Wong et al. conducted a retrospective analysis of 91 patients with advanced melanoma treated by anti-PD-1, including patients with an ECOG performance status of 2 and 3. Median age in the different groups was 54–73 years. They showed no statistically significant difference in irAEs between the groups with a low vs. high ECOG performance status. They did show that 81% of patients in the ECOG 2–3 group received anti-PD-1 therapy in the last month of life, compared with 46% in the ECOG 0-1 group [relative risk (RR) 1.75, 95% CI 1.04–2.56; p = 0.019]. Ninety percent of the patients in the ECOG 2–3 group were admitted to the hospital in the last month of life, compared with 52% in the ECOG 0–1 group (RR 1.73, 95% CI 1.10–2.16, p = 0.009). The ECOG 2–3 group were also more likely to die in an acute hospital setting (62% vs. 23%. respectively; RR 2.68, 95% CI 1.17–6.51; p = 0.016) [48]. All hospitalisation within the last month of life was for the management of disease progression. The only apparent admission for treatment-related toxicity was the aforementioned case of the patient with pulmonary infiltrates post-anti-PD1.
Horvat et al. performed a retrospective study in 298 patients with metastatic melanoma treated with ipilimumab, with a median age of 65 years and an ECOG performance status of 0–1. Discontinuation of treatment because of an irAE was reported in 19% of patients, most commonly because of diarrhoea and hepatotoxicity. Thirty-five percent of patients required systemic corticosteroid treatment for an irAE and 10% of all patients required additional systemic immunosuppressive therapy, mostly infliximab [49].
Luciani et al. performed a multicenter retrospective analysis on patients aged ≥ 75 years with advanced NSCLC treated with anti-PD-1 therapy and showed in 72 patients with a median age of 77 years that irAEs grade 3–4 occurred in 14% of patients, but the majority of patients had an ECOG status of 0–1 (63%) [50]. Corral de la Fuente et al. retrospectively analysed 98 patients with advanced NSCLC treated with anti-PD-1 or anti-PD-L1 therapy. The mean age was 62 years and 27 patients (27.5%) were aged ≥ 70 years. They reported 30.6% irAEs, with no statistically significant difference between the older and younger patients. The grade of severity of the adverse events was not reported [51].
Verzoni et al. conducted a retrospective analysis of 389 patients with previously treated advanced or metastatic renal cell carcinoma treated with nivolumab, including 70 patients (18%) aged ≥ 75 years with an ECOG performance status of 0–1 in 93.6% of patients. Immune-related adverse events occurred in 20% of patients, but no age-stratified analyses were performed [52].
Muchnik et al. performed a retrospective study in older patients receiving PD-1 inhibitors for advanced-stage NSCLC. They included 75 patients, with a median age of 74 years and 17 (22.7%) of the patients were aged ≥ 80 years. The Charlson Comorbidity Index was ≥ 3 in 40 (53.3%) patients and 37 (49.3%) patients had an ECOG performance status of ≥ 2. Overall, 37% of the patients experienced irAEs of any grade and 8% were grade ≥ 3 irAEs. Of these patients, 64% required treatment with glucocorticoids. The most common irAEs were pneumonitis, thyroiditis (both 12%), colitis and dermatitis (both 9%). Moreover, they showed that 64 patients discontinued treatment, 15% because of irAEs. During treatment, 54 (72%) patients were hospitalised, seven patients because of irAEs. The authors found no significant difference in irAE rates between different age, Charlson Comorbidiy Index or ECOG performance status groups [53].
Finally, Silva et al. performed a retrospective study in 106 elderly patients treated with immune checkpoint inhibitors for solid malignancies, with a mean age of 74.4 years. They found a similar irAE profile as previously reported. Remarkably, they found that frailty was the only statistically significant variable associated with the development of adverse events [54].
Treatment of Immune-Related Adverse Events in Older Patients
Because irAEs are caused by an excessive immune response, most of these are treated by withholding the immune checkpoint inhibitor or inducing temporary immunosuppression with oral glucocorticoids or additional immunosuppressants [29]. Most irAEs are mild and can be treated symptomatically [30]. To our knowledge, there are no studies on how to treat irAEs specifically in older patients.
According to the European Society for Medical Oncology (ESMO) guidelines, grade 1 and some grade 2 toxicities are mostly treated by withholding immune checkpoint inhibitors while monitoring symptoms and starting symptomatic or local treatment. Grade 3 and 4 toxicities, and some grade 2, are primarily treated with corticosteroid therapy. In the case of no improvement, other immunosuppressive drugs such as mycophenolate mofetil, infliximab (anti-tumour necrosis factor-α), tacrolimus, cyclophosphamide or anti-thymocyte globulin are recommended as additional therapy [32].
The use of some symptomatic treatments, such as antihistamines for pruritus or corticosteroids can be considered, but these may induce more extra adverse events in elderly patients, such as mental status disturbance, delirium, sodium and fluid retention, hypertension and worsening of diabetes mellitus [30]. Patients with comorbidities such as diabetes mellitus, congestive heart failure or underlying mood disorders may be at a higher risk for adverse events.
Discussion
In summary, the current available data show no difference in OS and PFS in older patients compared to younger patients and no major increase in irAE incidence in older patients. These data are mainly based on clinical trials, in which the elderly, especially aged ≥ 75 years, are underrepresented. There are no studies on how to treat irAEs specifically in older patients.
Most of the previously published immunotherapy trials did not perform any subanalyses in the different age groups. Moreover, because of strict inclusion criteria, only patients with a relatively good performance status and few comorbidities were enrolled in these trials. Hence, older patients with reduced functional reserve, or age-related comorbidities including autoimmune diseases and impaired organ function were excluded. The patients included are therefore not representative for the general older population of patients with cancer, which limits the evidence for treatment with immunotherapy in this population.
Interestingly, some of the subgroup analysis of trial data showed a higher incidence of irAEs and a trend towards early treatment discontinuation and a higher incidence of irAEs requiring treatment with immune-modulating medication in older patients [21, 38]. Moreover, Herin et al. showed an increased incidence of grade 1–2 irAEs and early occurrence of irAEs in older patients. This can be of consequence for older patients. For example, immune-related diarrhea may lead to a higher incidence of dehydration, decline in renal function and hospitalisation. Hospitalisation may have a different impact on older patients compared with younger patients. In addition, occurrence of multiple grade 1–2 irAEs may be a reason to discontinue therapy, which thereby hampers the efficacy of treatment.
We highlighted 12 observational studies in more real-life older patients than included in clinical trials, but still mainly patients with a good performance status. Previous clinical trials comparing chemotherapy with immune checkpoint inhibitors showed a higher incidence of chemotherapy-related grade 3–4 adverse events [42, 55], implicating that immune checkpoint inhibitors might be well tolerated by elderly patients. The observational studies we cited overall did not show an increased incidence of irAEs. However, some of the included studies showed a trend of a higher incidence of irAEs in older patients. As these studies were performed retrospectively and included a small number of patient, differences in the number of irAEs might not have been detected owing to bias or a lack of power. Furthermore, Muchnik et al. showed that a large proportion of the patients required treatment with glucocorticoids, discontinued treatment and were hospitalised. Moreover, the study of Wong et al. did show an increase in patients discontinuing therapy and more hospital admissions with increasing performance status. This suggests that the incidence of adverse events could be higher in patients with impaired physical functioning. The study also showed that more patients with a decreased performance status received immune checkpoint blockade therapy in the last month of life and were more likely to die in an acute hospital setting, which emphasises the importance of a more precise selection of patients receiving therapy.
It must be noted that the impact of irAEs in elderly patients may be greater than in younger patients, owing to age-related comorbidities and reduced functional reserve. For example, thyroiditis can result in either hypothyroidism or hyperthyroidism, which might worsen the symptoms of an undiagnosed neurocognitive disorder [33]. Interactions of adverse events and comorbidities may be problematic. For example, anticoagulants or anti-aggregants may increase the risk of gastrointestinal haemorrhage in colitis or autoimmune thrombocytopenia [20, 30].
There are minimal data on the safety in patients with renal of hepatic insufficiency. In contrast to chemotherapy, efficacy and safety of immune checkpoint inhibitors are thought to be similar in patients with renal or hepatic insufficiency because they are not cleared by the kidneys or liver [29]. Therefore, at the moment no dose adjustment is recommended [30]. In addition, adverse events are mostly not dose dependent, apart from the development of irAEs in patients receiving CTLA-4 inhibitors [56].
In the treatment of irAEs, the additional adverse events induced by corticosteroids or infliximab, as well as the effect of hospitalisation on elderly patients must be taken into consideration. Although long-term glucocorticoid therapy is not frequently needed, it may lead to additional complications, such as osteoporosis, glaucoma, cushingoid phenotype, opportunistic infections and proximal muscle weakness [29, 57]. Del Castillo et al. performed a retrospective study in 790 patients with advanced melanoma treated with an immune checkpoint blockade, assessing the risk of serious infections. They showed that the major risk factor for development of a serious infection was the use of immunosuppressive agents, including corticosteroids and infliximab (13.5% risk of serious infection vs. 2%) [58]. Therefore, the duration of corticosteroid usage should be limited, especially in older patients.
Furthermore, in the case of high-dose corticosteroid treatment, elderly patients are at increased risk of skin atrophy. Extra caution should also be taken when using high-dose corticosteroid treatment in elderly patients with underlying gastritis or undiagnosed peptic ulcer disease [33].
Frail patients are at increased risk of chemotherapy intolerance, postoperative complications and mortality [59]. Selecting frail patients using a geriatric assessment can help personalise treatment decisions. Remarkably, only one of the highlighted studies showed that frailty was associated with the development of adverse events. None of the other studies provided data on comprehensive geriatric assessments and measures of frailty. The ECOG and Karnofsky performance status generally overestimate physical functioning of older patients and as a result, these measurements are not valid to predict treatment toxicity [3]. The International Society of Geriatric Oncology therefore states that geriatric assessment can be valuable in clinical practice for the detection of impairments that were not identified in routine history or physical examination. Furthermore, it has been shown to predict severe treatment-related toxicity [3], and has been associated with survival outcomes [60–62]. Previous studies have shown that when a geriatric assessment is performed, it affects treatment choice and intensity [60]. The recommendation of the International Society of Geriatric Oncology (SIOG) is to evaluate the following domains: functional status, comorbidity, cognition, mental health status, fatigue, social status and support, nutrition and the presence of geriatric syndromes. However, the expert panel could not recommend one tool over another [2]. The G8 screening tool can help identify frail older patients with cancer requiring geriatric assessment and tailoring of cancer treatment [63, 64]. However, under-treatment of fit older patients might also be prevented in this manner. The ELDERS study is now comparing elderly patients to non-elderly patients receiving immunotherapy for lung cancer or melanoma, also gathering information about the comorbidity score and a geriatric screening assessment. Gomes et al. presented preliminary results of 32 patients with a minimum of 3 months follow-up. They found no statistically significant correlation between higher comorbidity score or abnormal geriatric assessment and the incidence of irAEs and found no significant negative impact on the global health-related quality of life [65]. Unfortunately, these finding are in a small group of patients with a limited follow-up and the final data are not presented yet. To our knowledge, to date, this is the only study evaluating the role of geriatric assessment in older patients receiving immune checkpoint inhibitors, highlighting the importance of future studies in this field.
Furthermore, traditional therapeutic studies rarely include functionality or quality of life as an endpoint, despite the fact that many older adults prioritise it as an important factor in the decision-making process [66]. The effect of immunotherapy on functional status can be critical for older adults, especially if it affects their ability to live independently. Therefore, more real-life-based data on adverse events and the effects on quality of life or effects on functional status can help in shared treatment decision making [67].
Conclusions
The clinical trials showed no age-dependent efficacy difference for immune checkpoint inhibitors. Overall, the incidence of treatment toxicity in older patients is higher in chemotherapy than immune therapy and clinical trials showed no major increase in irAE incidence with increasing age. However, in real life, studies in older and more vulnerable patients showed a higher incidence of irAEs, a trend to early treatment discontinuation and more patients requiring treatment with immune-modulating medication. The available observational data are limited. Because the enrolled elderly patients are not representative, further prospective studies should include older patients in a representative real-life population. Furthermore, future studies should include a geriatric assessment to identify which patients will benefit from immune checkpoint inhibitors and which patients are at higher risk of irAEs, hospitalisation and functional decline, and therefore might not benefit from immune checkpoint inhibitors.
Compliance with Ethical Standards
Funding
No external funding was used in the preparation of this article.
Conflict of Interest
Ellen Kapiteijn is on the advisory board of BMS and Merck. Yara van Holstein, Esther Bastiaannet, Frederiek van den Bos, Johanneke E.A. Portielje and Nienke A. de Glas have no conflicts of interest that are directly relevant to the content of this article.
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