Prevention of Chemotherapy-Induced Nausea and Vomiting in the Older Patient: Optimizing Outcomes.

Chemotherapy-induced nausea and vomiting (CINV) are still two of the most feared side effects of cancer therapy. Although major progress in the prophylaxis of CINV has been made during the past 40 years, nausea in particular remains a significant problem. Older patients have a lower risk of CINV than younger patients, but are at a higher risk of severe consequences of dehydration and electrolyte disturbances following emesis. Age-related organ deficiencies, comorbidities, polypharmacy, risk of drug-drug interactions, and lack of compliance all need to be addressed in the older patient with cancer at risk of CINV. Guidelines provide evidence-based recommendations for the prophylaxis of CINV, but none of these guidelines offer specific recommendations for older patients with cancer. This means that the recommendations may lead to overtreatment in some older patients. This review describes the development of antiemetic prophylaxis of CINV focusing on older patients, summarizes recommendations from antiemetic guidelines, describes deficiencies in our knowledge of older patients, summarizes necessary precautions, and suggests some future perspectives for antiemetic research in older patients.

Key Points

Introduction

Approximately 19.3 million new cancer cases were diagnosed worldwide in 2020. This number is expected to increase to 28.4 million cases in 2040 [1]. Cancer is primarily a disease in older people and the number of individuals aged ≥ 70 years diagnosed with cancer worldwide was approximately 7.2 million (37% of all cases) in 2020 and is expected to increase to 13.6 million new cancer cases in 2040, representing 48% of all new cases in 2040 [2]. This will have substantial economic and social impact. The fact that patients live longer after a cancer diagnosis will add to this burden [3].

Older patients present clinicians with challenges requiring knowledge and skills related to the complexities of managing multiple conditions concurrently. Issues like age-related organ deficiencies, comorbidity, polypharmacy, and frailty have the potential to influence decisions on anti-cancer treatment and supportive care [4]. It is therefore of great importance that oncologists are skilled in treating cancer and treatment-related complications in the elderly.

Chemotherapy-induced nausea and vomiting (CINV) are still two of the most feared side effects of cancer therapy, but significant progress in prophylaxis and treatment has been made over the past 40 years [5]. Older patients seem to have a lower risk of CINV than younger patients [6], but on the other hand they are at a higher risk of severe consequences (e.g., dehydration, electrolyte disturbances) associated with CINV. In this review, we will discuss the specific circumstances of CINV focusing older patients with cancer.

Risk Factors for Chemotherapy-Induced Nausea and Vomiting (CINV)

Chemotherapy-Related Risk Factors

The emetic potential of antineoplastic drugs is defined by the Multinational Association of Supportive Care in Cancer as high (> 90%), moderate (30–90%), low (10–30%), and minimal (< 10%) risk of emesis within the first 24 h after initiating chemotherapy. Except for the combination of an anthracycline and cyclophosphamide (AC), classified as high risk, the risk classification concerns only single antineoplastic drugs [7]. Patients are today exposed to a range of antineoplastic drugs across the emetic risk categories such as classical cytostatics, targeted agents, and immune therapy. Fortunately, targeted agents and immune therapy are most often classified as minimal emetic risk or low emetic risk agents. An exception to this is the poly (ADP ribose) polymerase (PARP) inhibitors, which often cause nausea and sometimes vomiting in the first months after start of treatment. Doses of chemotherapy are often reduced in the elderly [8], but except for a few drugs, guidelines do not distinguish between chemotherapy doses when defining emetic risk potentials.

Patient-Related Risk Factors

Several patient-related factors affect the risk of CINV.

Age

A number of studies show that older patients have a lower risk of CINV than younger patients. This is reported both when age is set at a threshold (e.g., 60 years) [9] or as a continuous variable [10]. However, the impact of chemotherapy-related side effects such as vomiting is greater in the elderly.

Gender

In randomized trials, women persistently have a higher risk of CINV than men [11, 12]. The reason for this is unknown.

Previous CINV

Patients who have experienced nausea and/or vomiting during previous courses of chemotherapy are at an increased risk of CINV in subsequent cycles [6, 12]. In addition, a history of CINV with previous chemotherapy has been shown to increase the risk of CINV with current chemotherapy [13].

Other Patient-Related Risk Factors

Low alcohol intake, anxiety, anticipation of CINV, emesis in pregnancy, and motion sickness are all additional individual risk factors for CINV [12, 14, 15].

Anti-emetic Prophylaxis

Adherence to guidelines has been shown to increase the control of CINV in patients receiving chemotherapy with high or moderate emetic risk [16]. Optimal prophylaxis with antiemetics reduces the risk of acute emesis with cisplatin from almost 100% to 10–20%.

Considerations When Prescribing Chemotherapy and Anti-emetics for Older Cancer Patients

Physiology of the Elderly

There is no universal definition of old age, but geriatric oncology is commonly defined as cancer in individuals aged 70 years or older [17]. Chronological age is, however, less important than biological age, because older people differ significantly in terms of physiological and psychological age-related ability. Individual assessment of suitability for cancer treatment and supportive care is therefore mandatory, rather than assessment based on chronological age alone [18].

Several age-related impairments should be considered in older patients with cancer. A change in drug absorption with ageing can be due to decreased esophageal, gastric, and colonic motility and/or to degeneration of villi in the small intestine [19].

Drug metabolism may be decreased by reductions in liver volume or cytochrome P450 enzymes, leading to increased bioavailability of some drugs. Reduced liver function may result in less protein binding of drugs, increasing the fraction of active drug. For example, the dose-adjusted exposure of the antiemetic olanzapine increases with age after oral administration, resulting in increased serum levels of olanzapine in older compared with younger adults [20]. This may explain the higher risk of sedation in older patients receiving olanzapine [5].

The glomerular filtration rate (GFR) normally declines from the fourth decade by around 1% per year [21, 22]. This has implications for dosing and drug toxicity. While GFR can be easily estimated based on serum creatinine in younger patients, these estimations are often inaccurate in the elderly [23], meaning that the gold standard in older patients with cancer should be direct measurement of exogenous filtration markers such as 51Cr-EDTA.

Aging results in a decline in diastolic function and cardiac reserve due to left ventricular wall thickening as well as an increased prevalence of atrial fibrillation [24]. Examples of age-related heart disorders to consider are heart failure and arrhythmias, which may impact decisions regarding anticancer therapy and supportive care medications. In particular, QTC prolongation should be considered because this is a class adverse effect of the antiemetic group of 5-HT3-receptor antagonists [25].

Bone marrow and bone density changes occur frequently in the elderly. The most apparent change in bone marrow function is decreased cellularity, estimated to be only 30% in those aged ≥ 65 years as compared with younger people [26]. This likely contributes to the increased risk of chemotherapy-induced neutropenia [27] and thrombocytopenia observed in older patients with cancer.

Age-related cognitive impairment can be aggravated by cancer and antineoplastic therapy [28]. Difficulties with short-term memory can result in non-adherence to oral drug therapy [29]. Consequently, simple antineoplastic and antiemetic treatment regimens may be preferred in order to optimize compliance.

Comorbidity

Comorbidity in cancer patients is defined as the occurrence or the existence of any distinct additional medical condition to cancer [30]. Two in three older adults (aged 65 years or more) have at least one comorbidity and the number of comorbidities increases with age. Approximately 40% and 13% of older adults have three or more and five or more comorbidities, respectively [30]. It is known that older patients with cancer have a higher prevalence of comorbidity than an age-matched control group without cancer [31]. Also, the number and type of comorbidities differ with the type of cancer [31]. The difference in prevalence according to cancer diagnoses is likely explained by overlapping risk factors associated with both comorbidity and cancer; for example, smoking is a risk factor for both chronic obstructive pulmonary disease and lung cancer. Some of the most common comorbidities in patients with cancer are hypertension, cardiovascular disease, musculoskeletal or joint disease, diabetes mellitus, and pulmonary disease [32]. Different scales have been developed and validated to measure comorbidity burden, such as Charlson’s Comorbidity Index (CCI) [33] and the Cumulative Rating Scale for Geriatrics [34]. When assessing cancer patients with comorbidity it is important to address how the comorbidity might affect prognosis, the impact of comorbidity on anticancer and supportive care therapy, and the potential effects of anticancer and supportive care therapy on comorbid diseases.

Polypharmacy

There is no consensus on the definition of polypharmacy, but the most frequently used define polypharmacy as the use of five or more medications [35]. Due to increased prevalence of multi-morbidity, physiological changes, and functional limitations, older patients with cancer have a high risk for polypharmacy, adverse drug reactions, and potentially inappropriate medications [36, 37]. In a study of patients newly diagnosed with cancer and aged 70 + years, 35% used five or more prescription medications daily [38]. The addition of non-prescription medication, antineoplastic agents, and supportive care agents (like antiemetics) will increase this number significantly. Polypharmacy results in high risk of potential drug–drug interactions that may have major implications for older patients with cancer, such as an increased risk of unplanned hospitalization [39]; consequently, antiemetics with a low risk of drug–drug interactions should be preferred in older patients with cancer.

Antiemetics

Until the 1960s, treatment of CINV was carried out on an empirical basis. CINV studies in the years 1960–1980 primarily included dopamine2-receptor antagonists or cannabinoids, but study methodology did not meet the requirements of today and only the first 24 h after initiation of chemotherapy were studied.

During the next 15 years (1980–1995), the primary focus was on studies with corticosteroids and serotonin (5-HT)3-receptor antagonists. In particular, methodology of the 5-HT3-receptor antagonist studies was improved and the study period often prolonged to include the first 5 days after chemotherapy.

The studies from 1995 to today have concentrated on the development of neurokinin (NK)1-receptor antagonists and lately on the multi-receptor targeting agent, olanzapine.

Dopamine (D)2,3-Receptor Antagonists

Dopamine was described as a brain neurotransmitter in 1957 [40]. Dopamine receptors are divided into five groups (D1–D5 receptors), but only D2 and D3 receptors seem to be involved in the emesis pathway [41, 42]. Numerous D2-receptor antagonists have been studied, such as phenothiazines (metopimazine and prochlorperazine), butyrophenone (haloperidol), the substituted benzamide (metoclopramide), and the benzimidazole derivative (domperidone). The D2-receptor antagonists are not included in the fixed antiemetic regimens of the evidence-based guidelines of today [5], but are only recommended as rescue antiemetics. Recently, the D3-receptor antagonist, amisulpride, has been investigated in CINV [43].

Metopimazine

Metopimazine was investigated by Moertel and Reitemeier in two randomized, double-blind studies. In the first study, metopimazine 5 mg × 3 orally was equal to metoclopramide 20 mg × 3 orally, but none of the drugs were superior to placebo [44]. In the second study, metopimazine (15 mg × 3 orally) was equal to prochlorperazine but with less sedation, and both were superior to placebo [45]. Based on these studies, it was suggested to investigate metopimazine in higher doses. In two subsequent studies, it was then demonstrated that metopimazine in doses of 30 mg × 4 orally increases the antiemetic effect of the 5-HT3-receptor antagonist, ondansetron, in CINV [46, 47]. In contrast to the majority of the other D2-receptor antagonists, metopimazine does not induce extrapyramidal adverse effects because of its low penetration of the blood–brain barrier [48]. Metopimazine delays gastric emptying, and constipation is therefore an adverse event in 10–20% of patients. Unfortunately, metopimazine is not globally available and therefore of only limited research interest.

Prochlorperazine

Prochlorperazine is superior to placebo against CINV induced by chemotherapy of low and moderate emetic risk [44] and inferior [49] or equal to metoclopramide [50]. A number of studies have compared prochlorperazine to a cannabinoid, but primarily in patients who were refractory to prochlorperazine in previous courses of chemotherapy, meaning that no conclusions can be drawn [51]. A recent study has demonstrated activity of prochlorperazine in combination with dexamethasone against delayed CINV [52].

Metoclopramide

Metoclopramide is the D2-receptor antagonist that is best studied. It is a substituted benzamide derived from procainamide (methoxychloroprocainamide) and was first described by Justin-Besancon in 1964 [53]. Metoclopramide was effective against nausea and vomiting induced by a number of non-malignant conditions [54]. In low doses (20 mg × 2–3, orally), metoclopramide was no better than placebo [44] and inferior to dexamethasone and domperidone [55]. The interest in investigating metoclopramide further was therefore modest until Gralla and coworkers [56] demonstrated the significant effect of high-dose metoclopramide (2 mg/kg intravenously [IV] × 5) against cisplatin-induced nausea and vomiting. Subsequent studies optimized the high-dose metoclopramide regimen, by comparing the 2 mg/kg IV × 5 regimen with a continuous infusion [57] or with two IV bolus infusions only [58, 59]. Acute dystonic reactions induced by high-dose metoclopramide were a significant problem, but the addition of diphenhydramine or lorazepam resulted in a significant reduction in the incidence of extrapyramidal adverse effects [58]. A modified high-dose metoclopramide regimen (3 mg/kg IV × 2 or 4 mg/kg IV × 1) combined with dexamethasone and lorazepam or diphenhydramine (to decrease the incidence of extrapyramidal adverse effects) became the standard antiemetic regimen in cisplatin-based chemotherapy [58] until the early 1990s. Metoclopramide has a prokinetic effect on the GI tract, and diarrhea is therefore a frequent adverse effect. It was soon verified that the antiemetic effect of high-dose metoclopramide was not caused by antagonism at D2-receptors, but was caused by antagonism at 5-HT3-receptors [60-63]. This led to the development of a new class of antiemetic agents, the serotonin-receptor antagonists.

Domperidone

Domperidone was investigated in high doses in a number of studies in the 1980s in order to explore a possible dose–effect relationship like the one seen with metoclopramide. Unfortunately, high doses of domperidone induced cardiac adverse effects (cardiac arrest and sudden death) in a number of patients [64-67]. Consequently, the parenteral formulation was withdrawn from general use. In low IV doses or oral doses of 20 mg × 3, domperidone was superior to placebo [68], inferior [69] or superior [55] to metoclopramide, and inferior [69] or equal to dexamethasone [55]. Like metoclopramide, domperidone has a prokinetic effect on the GI tract and diarrhea is a frequent adverse effect. Extrapyramidal adverse effects are rarely seen, because the penetration of the blood–brain barrier is limited [48].

Corticosteroids

The first randomized double-blind study was published in 1979 and concluded that dexamethasone was superior to placebo in patients receiving non-cisplatin chemotherapy [70]. Subsequent studies supported the finding that single-agent corticosteroids possess an antiemetic effect in patients receiving chemotherapy with low and moderate emetic risk [55, 71]. When prescribed to patients receiving chemotherapy with moderate or high emetic risk, corticosteroids improve the effect of other antiemetics such as the 5-HT3-receptor antagonists [72, 73]. Dexamethasone is the best investigated agent, but there is no reason to believe that there are major differences between dexamethasone and prednisolone. Recently, a number of studies have compared a 1-day regimen of dexamethasone with a 3-day regimen (‘steroid-sparing regimens’). In patients receiving carboplatin-based or AC-based chemotherapy and a three-drug combination as antiemetic prophylaxis (a 5-HT3-receptor antagonist, a NK1-receptor antagonist, and dexamethasone), no major differences were observed between the 1-day and 3-day regimens of dexamethasone. This is also acknowledged in the recently published guidelines (see Sects. 5.3 and 5.4).

Serotonin (5-HT)3-Receptor Antagonists

Serotonin (5-HT) was discovered in 1948. 5-HT receptors are divided into seven groups (5-HT1–5-HT7) with 5-HT3 receptors as the most important in the emesis pathway. The 5-HT3-receptor antagonists are the most effective antiemetics in the prophylaxis of acute nausea and vomiting (0–24 h after initiation of chemotherapy), whereas the effect against delayed nausea and vomiting (24–120 h after initiation of chemotherapy) is modest. There are only minor differences between the 5-HT3-receptor antagonists as concerns effect and tolerability. A large number of 5-HT3-receptor antagonists have been marketed, but only the most frequently used (ondansetron, granisetron, and palonosetron) will be addressed. The first two clinical studies were published in 1987 [74, 75]. The most important studies are summarized in Tables 1, 2 and 3.

Table 1

Key trials in the development of the serotonin (5-HT)3-receptor antagonist ondansetron

References	Design	Investigational arm	Comparator	Chemotherapy	Primary parameter	Result
Cubeddu et al. [76]	R, DB, P n = 28	OND 0.15 mg/kg × 3 IV	PLA × 3 IV	CIS-based	Number of EE 0–24 h	OND > PLA
Marty et al. [78]	R, DB, CO n = 97	OND 8 mg IV + OND 1 mg/h IV 0–24 h	MCP 3 mg/kg IV + MCP 0.5 mg/kg/h for 0–8 h	CIS-based	Number of EE 0–24 h, treatment preference	OND > MCP
Bonneterre et al. [79]	R, DB, CO n = 75	OND 4 mg IV + OND 4 mg PO on day 1 + OND 8 mg × 3 PO for 3–5 days	MCP 60 mg IV + MCP 20 mg PO on day 1 + MCP 20 mg × 3 PO for 3–5 days	AC-based	Complete or major control of emesis (0–2 EE) 0–24 h, treatment preference	0–24 h: OND > MCP both emesis and nausea Day 2–3: OND > MCP only emesis not nausea
Kaasa et al. [80]	R, DB, P n = 82	OND 8 mg IV on day 1 + OND 8 mg × 3 PO for 3–5 days	MCP 60 mg IV + MCP 20 mg PO × 3 for 3–5 days	AC-based	Number of EE 0–24 h	Acute: OND > MCP Delayed: no significant difference
Cubeddu et al. [77]	R, DB, P n = 20	OND 0.15 mg/kg × 3 IV	PLA × 3 IV	C-based	Number of EE 0–24 h	OND > PLA
Marschner et al. [81]	R, DB, P n = 122	OND 8 mg PO + OND 8 mg × 3 PO for 3–5 days	MCP 60 mg IV + MCP 20 mg PO × 3 for 3–5 days	AC-based	Complete or major control of emesis (0–2 EE) 0–24 h	No significant difference
Jones et al. [82]	R, DB, CO n = 112	DEX 8 mg IV on day 1 + DEX 4 mg × 4 PO on days 1–2, 2 mg × 4 PO on days 3–4, 1 mg × 4 PO on day 5	OND 4 mg IV on day 1 + OND 4 mg × 4 PO on days 1–5	AC-based or MEC	Complete or major control of emesis (0–2 EE) 0–24 h, treatment preference	Emesis: DEX = OND Delayed nausea: DEX > OND

A anthracycline, C cyclophosphamide, CIS cisplatin, CO cross-over, DB double-blind, DEX dexamethasone, EE emetic episodes, IV intravenously, MCP metoclopramide, MEC moderately emetogenic chemotherapy, O open label, OND ondansetron, P parallel, PLA placebo, PO orally, R randomized

Table 2

Key trials in the development of the serotonin (5-HT)3-receptor antagonist granisetron

References	Design	Investigational arm	Comparator	Chemotherapy	Primary parameter	Result
Warr et al. [83]	R, DB, P n = 152	GRA 80 μg/kg IV	PCP 10 mg IV + DEX 10 mg IV	Dactinomycin, CIS, AC, or MEC	Severity of nausea and number of EE 0–24 h	GRA > PCP + DEX
Warr et al. [84]	R, DB, P n = 149	GRA 80 μg/kg IV	DEX 10 mg IV + DPH 10 mg IV + MCP 2 mg/kg IV every 2 h for 5 doses	CIS	Severity of nausea and number of patients with no EE 0–24 h	GRA = DEX + MCP + DPH
Perez et al. [85]	R, DB, P n = 1085	GRA 2 mg PO ± DEX	OND 32 mg IV ± DEX	Primarily carboplatin or C	Total control (no EE, no nausea, no rescue medications) 0–24 h and 25–48 h	GRA = OND
Gralla et al. [86]	R, DB, P n = 1054	GRA 2 mg PO ± DEX	OND 32 mg IV ± DEX	CIS	Total control (no EE, no nausea, no rescue medications) 0–24 h	GRA = OND
Raftopoulos et al. [87]	R, DB, P n = 1395	Sustained-release GRA 250 µg or 500 µg subcutaneously	PAL 0.25 mg IV	HEC/MEC	Complete response (no EE, no rescue medications) 0–24 h	Both doses of GRA noninferior to PAL

A anthracycline, C cyclophosphamide, CIS cisplatin, DB double-blind, DEX dexamethasone, DPH diphenhydramine, EE emetic episodes, GRA granisetron, HEC highly emetogenic chemotherapy, IV intravenously, MCP metoclopramide, MEC moderately emetogenic chemotherapy, OND ondansetron, P parallel, PAL palonosetron, PCP prochlorperazine, PLA placebo, PO orally, R randomized

Table 3

Key trials in the development of the serotonin (5-HT)3-receptor antagonist palonosetron

References	Design	Investigational arm	Comparator	Chemotherapy	Primary parameter		Result
Gralla et al. [88]	R, DB, P n = 563	a) PAL 0.25 mg IV b) PAL 0.75 mg IV	OND 32 mg IV	Low-dose CIS, various MEC	Complete response (no EE, no rescue medication) 0–24 h		Both doses of PAL noninferior to OND
Eisenberg et al. [89]	R, DB, P n = 569	a) PAL 0.25 mg IV b) PAL 0.75 mg IV	DOL 100 mg IV	Low-dose CIS, AC or various MEC	Complete response (no EE, no rescue medication) 0–24 h		Both doses of PAL noninferior to DOL
Aapro et al. [90]	R, DB, P n = 667	a) PAL 0.25 mg IV ± DEX 20 mg IV b) PAL 0.75 mg IV ± DEX 20 mg IV	OND 32 mg IV ± DEX 20 mg IV	Various HEC, primarily CIS	Complete response (no EE, no rescue medication) 0–24 h		Both doses of PAL noninferior to OND
Saito et al. [91]	R, DB, P n = 1119	PAL 0.75 mg IV + DEX 16 mg IV on day 1 + DEX 8 mg IV (CIS) or 4 mg PO (AC) ×1 on days 2–3	GRA 40 µg/kg IV + DEX 16 mg IV on day 1 + DEX 8 mg IV (CIS) or 4 mg PO (AC) ×1 on days 2–3	CIS or AC	Complete response (no EE, no rescue medication) 0–24 h and 25–120 h		PAL + DEX noninferior 0–24 h and PAL + DEX superior to GRA + DEX 25–120 h

A anthracycline, C cyclophosphamide, CIS cisplatin, DB double-blind, DEX dexamethasone, DOL dolasetron, EE emetic episodes, GRA granisetron, HEC highly emetogenic chemotherapy, IV intravenously, MEC moderately emetogenic chemotherapy, OND ondansetron, P parallel, PAL palonosetron, PLA placebo, PO orally, R randomized

Ondansetron

Ondansetron was initially compared with single antiemetic agents and found to be superior to placebo in the prophylaxis of CINV induced by high-risk [76] and moderate emetic risk [77] chemotherapy and to high-dose metoclopramide in prophylaxis of CINV induced by chemotherapy with high emetic risk [78]. In patients receiving chemotherapy with moderate emetic risk, ondansetron was either superior [79, 80] or equal to [81] metoclopramide in the prophylaxis of acute nausea and vomiting, but without any significant difference in the delayed phase. A study compared ondansetron with dexamethasone in patients treated with moderate emetic risk chemotherapy and concluded that both antiemetics were equal in prevention of acute nausea and vomiting, whereas dexamethasone was superior in prophylaxis of delayed nausea [82]. As previously mentioned, dexamethasone improves the effect of ondansetron [72].

Granisetron

In contrast to the development of ondansetron, granisetron was initially compared with antiemetic combination regimens. In patients receiving moderate emetic risk chemotherapy, granisetron was superior to a combination of prochlorperazine and dexamethasone in the prophylaxis of acute emesis [83], and granisetron was as effective as a combination of high-dose metoclopramide, dexamethasone, and diphenhydramine in patients receiving cisplatin-based chemotherapy with high emetic risk [84]. As for the other 5-HT3-receptor antagonists, the effect is improved by the addition of dexamethasone [73]. Two large randomized, double-blind studies compared oral granisetron with intravenous ondansetron [85, 86] and found no differences in efficacy and tolerability. In a subsequent randomized, double-blind study, extended-release granisetron was noninferior to palonosetron [87].

Palonosetron

Palonosetron was marketed in 2003 (more than 10 years after ondansetron and granisetron), and the phase III pivotal trials consequently used a noninferiority design and compared palonosetron with two of the older 5-HT3-receptor antagonists. Two randomized, double-blind studies in patients receiving single-agent chemotherapy with moderate emetic risk or AC or low-dose cisplatin (< 50 mg/m2) compared palonosetron with ondansetron [88] and dolasetron [89], respectively. Palonosetron was statistical significantly superior to ondansetron [88] and noninferior to dolasetron [89] in terms of patients with a complete response (CR) in the acute phase (no emesis and no need for other antiemetics 0–24 h after initiation of chemotherapy). In a third study, palonosetron was noninferior to ondansetron in prevention of acute nausea and vomiting in patients receiving cisplatin-based, high-emetic-risk chemotherapy [90]. In contrast to the two previously mentioned studies [88, 89], 67% of patients in both study arms received dexamethasone. In a large, randomized, double-blind, phase III post-marketing trial, palonosetron plus dexamethasone was compared with granisetron plus dexamethasone in patients receiving high-emetic-risk chemotherapy [91]. Palonosetron plus dexamethasone was noninferior to granisetron plus dexamethasone in the acute phase, but superior in the delayed phase.

Adverse Effects and Potential Drug–Drug Interaction Risks

The 5-HT3-receptor antagonists are generally well tolerated, with constipation, headache, slight reversible increase in liver transaminases, and QTC prolongation as drug class adverse effects. The 32-mg dose of ondansetron and the intravenous formulation of dolasetron were both withdrawn from the market due to FDA warnings (QTC prolongations). Palonosetron seems to have a low risk and did not cause QTc prolongation when investigated in 221 healthy volunteers, but the mean age of the volunteers was 41 years, which is approximately 25 years younger than the average cancer patient [92]. A few reports of palonosetron QTc prolongation [93] and ventricular tachycardia [94] have been published. The risk of 5-HT3-receptor antagonist-induced QTc prolongation is enhanced in older cancer patients, in particular if patients receive other agents with potential QTc prolongation risk.

The 5-HT3-receptor antagonists are metabolized through different pathways. Granisetron is metabolized through the CYP450 3A4 enzyme pathway, whereas ondansetron and palonosetron are primarily metabolized through the CYP 2D6 pathway. The CYP 2D6 pathway is subject to genetic polymorphisms, meaning that patients can have zero (poor metabolizers), one (normal), two (extensive metabolizers), or three (ultrarapid metabolizers) active CYP2D6 genes. From an antiemetic point of view, the ultrarapid metabolizers are the most interesting group, because lack of antiemetic effect has been described with tropisetron and ondansetron in these patients [95]. In this case, rotation to granisetron can be useful.

Neurokinin (NK)1-Receptor Antagonists

Substance P (neurokinin) was discovered in 1931, but was not sequenced and purified until 1970. Three neurokinin (NK) receptors were identified in the mid-1980s, of which the NK1 receptor is involved in the emetic reflex arch. The NK1-receptor antagonists have antiemetic effect in the prevention of both acute and delayed nausea and vomiting. A large number of NK1-receptor antagonists have been investigated, but only the three marketed oral agents, aprepitant, netupitant, and rolapitant, and their intravenous formulations will be reviewed. The first clinical study with one of these agents was published in 1997 [96]. The pivotal and other important studies are summarized in Tables 4, 5 and 6.

Table 4

Key trials in the development of the neurokinin (NK)1-receptor antagonist aprepitant

References	Design	Investigational arm	Comparator	Chemotherapy	Primary parameter	Result
Navari et al. [97]	R, DB, P n = 158	All: GRA 10 μg/kg IV + DEX 20 mg PO on day 1 a) APR 400 mg PO on day 1 +  APR 300 mg PO on days 2–5 b) APR 400 mg PO on day 1 c) PLA	GRA 10 μg/kg IV + DEX 20 mg PO on day 1 + PLA (arm c)	CIS	No EE, 25–120 h	APR > PLA
Chawla et al. [101]	R, DB, P n = 381	All: OND 32 mg IV + DEX 20 mg PO on day 1 + DEX 8 mg PO on days 2–5 a) APR 40 mg PO on day 1 + APR 25 mg PO on days 2–5 b) APR 125 mg PO on day 1 + APR 80 mg PO on days 2–5	OND 32 mg IV + DEX 20 mg PO on day 1 + DEX 8 mg PO on days 2–5 + PLA on days 1–5	CIS	Complete response (no EE, no rescue medication) 0–120 h	Both APR doses > PLA PLA 125/80 chosen for phase III studies (3-day regimen)
Hesketh et al. [102]	R, DB, P n = 521	APR 125 mg PO + OND 32 mg IV + DEX 12 mg PO on day 1 + APR 80 mg PO + DEX 8 mg PO on days 2–3 + DEX 8 mg PO on day 4	OND 32 mg IV + DEX 20 mg PO on day 1 + DEX 8 mg × 2 PO on days 2–4	CIS	Complete response (no EE, no rescue medication) 0–120 h	APR > PLA
Poli-Bigelli et al. [103]	R, DB, P n = 567	APR 125 mg PO + OND 32 mg IV + DEX 12 mg PO on day 1 + APR 80 mg PO + DEX 8 mg PO on days 2–3 + DEX 8 mg PO on day 4	OND 32 mg IV + DEX 20 mg PO on day 1 + DEX 8 mg × 2 PO on days 2–4	CIS	Complete response (no EE, no rescue medication) 0–120 h	APR > PLA
Warr et al. [105]	R, DB, P n = 866	APR 125 mg PO + OND 8 mg × 2 PO + DEX 12 mg PO on day 1 + APR 80 mg PO on days 2–3	OND 8 mg ×2 PO + DEX 20 mg PO on day 1 + OND 8 mg × 2 PO on days 2–3	AC-based	Complete response (no EE, and no rescue medication) 0–120 h	APR > PLA

A anthracycline, APR aprepitant, C cyclophosphamide, CIS cisplatin, DB double-blind, DEX dexamethasone, EE emetic episodes, GRA granisetron, IV intravenously, OND ondansetron, P parallel, PLA placebo, PO orally, R randomized

Table 5

Key trials in the development of the neurokinin (NK)1-receptor antagonist netupitant

References	Design	Investigational arm	Comparator	Chemotherapy	Primary parameter	Result
Hesketh et al. [109]	R, DB, P n = 677	a) NET 100 mg PO on day 1 b) NET 200 mg PO on day 1 c) NET 300 mg PO on day 1 d) APR 125 mg PO + OND 32 mg IV + DEX 12 mg PO on day 1 + APR 80 mg PO + DEX 4 mg × 2 PO on days 2–3 + DEX 4 mg × 2 PO on day 4 a-c: PAL 0.5 mg PO + DEX 12 mg PO on day 1 + DEX 4 mg × 2 PO on days 2–4	PAL 0.5 mg PO + DEX 20 mg PO on day 1 + DEX 8 mg × 2 PO on days 2–4	CIS	Complete response (no EE, no rescue medication) 0–120 h	NET + PAL + DEX > PAL + DEX + PLA in all doses NET 300 mg chosen for phase III studies
Aapro et al. [110]	R, DB, P n = 1449	NEPA (NET 300 mg + PAL 0.5 mg) PO + DEX 12 mg PO	PAL 0.5 mg + DEX 20 mg PO	AC	Complete response (no EE, no rescue medication) 24–120 h	NEPA + DEX > PAL + DEX
Gralla et al. [112]	R, DB, P n = 412	NEPA (NET 300 mg + PAL 0.5 mg) PO on day 1 + HEC: DEX 12 mg PO on day 1 + DEX 8 mg PO on days 2–4 MEC: DEX 12 mg PO on day 1	APR 125 mg PO + PAL 0.5 mg PO on day 1 + APR 80 mg PO on days 2–3 + HEC: DEX 12 mg PO on day 1 + DEX 8 mg PO on days 2–4 MEC: DEX 12 mg PO on day 1	HEC or MEC	Safety over multiple cycles	NEPA + DEX = APR + PAL + DEX, no increase in adverse events over multiple cycles

A anthracycline, APR aprepitant, C cyclophosphamide, CIS cisplatin, DB double-blind, DEX dexamethasone, EE emetic episodes, HEC highly emetogenic chemotherapy, IV intravenously, MEC moderately emetogenic chemotherapy, NEPA NET + PAL, NET netupitant, P parallel, PAL palonosetron, PO orally, R randomized

Table 6

Key trials in the development of the neurokinin (NK)1-receptor antagonist rolapitant

References	Design	Investigational arm	Comparator	Chemotherapy	Primary parameter	Result
Rapoport et al. [115]	R, DB, P n = 454	Day 1: a) ROL 9 mg PO b) ROL 22.5 mg PO c) ROL 90 mg PO d) ROL 180 mg PO All: OND 32 mg IV + DEX 20 mg PO on day 1 + DEX 8 mg × 2 PO on days 2–4	OND 32 mg IV + DEX 20 mg PO on day 1 + DEX 8 mg × 2 PO on days 2–4	CIS	Complete response (no EE, no rescue medication) 0–120 h	ROL + OND + DEX > OND + DEX, all doses except ROL 9 mg ROL 180 mg chosen for phase III studies
Rapoport et al. [116]	R, DB, P n = 1070	ROL 180 mg PO + GRA 10 µg/kg IV + DEX 20 mg PO on day 1 + DEX 8 mg × 2 PO on days 2–4	GRA 10 µg/kg IV + DEX 20 mg PO on day 1 + DEX 8 mg × 2 on days 2–4	CIS	Complete response (no EE, no rescue medication) 24–120 h	ROL + GRA + DEX > GRA + DEX
Schwartzberg et al. [117]	R, DB, P n = 1332	ROL 180 mg PO + GRA 2 mg PO + DEX 20 mg PO on day 1 + GRA 2 mg × 1 on days 2–3	GRA 2 mg PO + DEX 20 mg PO on day 1 + GRA 2 mg × 1 on days 2–3	AC or various MEC	Complete response (no EE, no rescue medication) 24–120 h	ROL + GRA + DEX > GRA + DEX

A anthracycline, APR aprepitant, C cyclophosphamide, CIS cisplatin, DB double-blind, DEX dexamethasone, EE emetic episodes, GRA granisetron, IV intravenously, MEC moderately emetogenic chemotherapy, OND ondansetron, P parallel, PLA placebo, PO orally, R randomized, ROL rolapitant

Aprepitant and Fosaprepitant

Aprepitant and the prodrug fosaprepitant were investigated in five randomized, double-blind, phase II trials using a 5-day aprepitant regimen [97-101]. Aprepitant was inferior to the 5-HT3-receptor antagonists, ondansetron and granisetron, against acute nausea and vomiting, but active in the prevention of delayed nausea and vomiting. In combination with either ondansetron plus dexamethasone or granisetron plus dexamethasone, aprepitant increased the antiemetic effect compared with placebo [101]. The phase II studies revealed a drug–drug interaction between aprepitant and dexamethasone (both metabolized through CYP3A4), resulting in an approximately 50% increase in plasma concentrations of dexamethasone [101]. Consequently, the phase III studies used a 3-day aprepitant regimen in lower dosages than used in phase II and the dosage of dexamethasone was reduced to 50–60% when combined with aprepitant. Two phase III studies in cisplatin-based chemotherapy compared ondansetron on day 1 plus dexamethasone on days 1–4 plus placebo on days 1–3 with ondansetron on day 1 plus dexamethasone on days 1–4 plus aprepitant on days 1–3 [102, 103], and a third study used the same methodology and comparison but added ondansetron on days 2–4 in the placebo arm [104]. All studies were randomized, double-blinded, and concluded that aprepitant increased the CR rate (no emesis and no need for rescue antiemetics) both in the acute and delayed phases of CINV. Two studies in patients receiving AC-based chemotherapy [105] or AC or chemotherapy with moderate emetic risk [106], respectively, compared ondansetron on day 1 plus dexamethasone on days 1–3 plus placebo on days 1–3 with ondansetron on day 1 plus dexamethasone on days 1–3 plus aprepitant on days 1–3. Both concluded that aprepitant was significantly superior to placebo as concerns CR on days 1–5 after chemotherapy. The first of these studies [105] included a multiple cycle extension part and demonstrated that the effect of aprepitant was maintained over four cycles of AC chemotherapy [107]. Finally, a large, randomized, double-blind study (n = 2.322) found that a single dose of fosaprepitant IV was noninferior to the standard 3-day regimen of oral aprepitant [108].

Netupitant and Fosnetupitant

Netupitant was investigated and developed in combination with palonosetron (NEPA) given as a single oral dose administered before chemotherapy. Three pivotal studies were conducted [109, 110, 112]. A dose ranging study in patients receiving cisplatin-based chemotherapy concluded that a single oral dose of NEPA plus dexamethasone on days 1–4 was superior to a single oral dose of palonosetron plus dexamethasone on days 1–4 and recommended the 300-mg netupitant dose for use in phase III trials [109].

A large, randomized, double-blind study (n = 1449) compared the antiemetic effect of NEPA + dexamethasone (12 mg) on day 1 with palonosetron plus dexamethasone (20 mg) on day 1 in patients receiving either AC chemotherapy or epirubicin + cyclophosphamide (EC). NEPA was superior to palonosetron in terms of CR in the delayed phase (primary parameter), but also in the acute and overall phase and as concerns no emesis and no significant nausea [110]. This study also included a multiple cycle extension in which 1286 of the 1449 patients participated. The antiemetic effect of NEPA was superior to palonosetron during all four cycles and no safety concerns were raised [111].

A phase III, randomized, double-blind study (n = 412) investigated a single dose of NEPA + dexamethasone (on day 1 in moderate-emetic-risk and days 1–4 in high-emetic-risk patients) during multiple cycles of chemotherapy [112]. The comparator arm included aprepitant on days 1–3 plus palonosetron on day 1 and dexamethasone as in the NEPA arm. The primary parameter was safety during multiple cycles. Patients received either a high-emetic-risk agent (e.g., cisplatin) or one of several moderate-emetic-risk agents (e.g., doxorubicin or cyclophosphamide, but not the combination). Seventy-five percent of the patients completed at least four cycles of chemotherapy and the incidence and type of adverse effects were comparable for both groups with no indication of increasing adverse events over multiple cycles.

A single infusion of fosnetupitant (IV NEPA) was compared with a single oral dose of NEPA (both combined with dexamethasone) in two randomized, double-blind trials including patients receiving a single high-emetic-risk agent [113] or AC chemotherapy [114], respectively. IV NEPA was as effective as oral NEPA and no treatment-related injection-site adverse effects or episodes of hypersensitivity or anaphylaxis were reported.

Rolapitant

Rolapitant was primarily investigated in a phase II dose-finding study [115] and in three randomized, double-blind, phase III trials, two in patients treated with cisplatin-based chemotherapy [116] and one in patients receiving AC/EC chemotherapy or different agents with moderate emetic risk [117].

The randomized, double-blind, dose-finding, phase II study included 454 patients all receiving cisplatin-based chemotherapy and ondansetron plus dexamethasone as antiemetic prophylaxis. Patients were randomized to one of four doses of rolapitant (9–180 mg) or to placebo. The greatest benefit was observed with the 180-mg dose of rolapitant, which consequently became the dose used in phase III trials [115]. Rolapitant was investigated in two (HEC-1 and HEC-2) phase III studies (identical except for the location of the participating sites) in patients receiving cisplatin-based (≥60 mg/m2) chemotherapy. All patients received granisetron IV (10 µg/kg) and dexamethasone 20 mg orally before chemotherapy plus dexamethasone 8 mg × 2 orally on days 2–4 and were randomized to receive placebo or rolapitant 180 mg on day 1 in addition (n = 526 in HEC-1 and 544 in HEC-2). The primary endpoint was CR (defined as no emesis and no rescue antiemetics) in the delayed phase (24–120 h after chemotherapy). Significantly more patients in the rolapitant group had CR as compared with the placebo-treated patients in HEC-1, HEC-2, and in the combined analysis of both studies with no significant differences in adverse effects [116].

In a third study, 1332 patients either received AC/EC chemotherapy or different agents with moderate emetic risk such as cyclophosphamide, an anthracycline, irinotecan, oxaliplatin, or carboplatin. All patients received granisetron 2 mg orally and dexamethasone 20 mg orally before chemotherapy and continued with granisetron 2 mg orally × 1 on days 2–3 and were randomized to rolapitant or placebo × 1 on day 1. A significantly higher proportion of patients in the rolapitant group as compared with the placebo group had CR in the delayed phase (primary effect parameter) with no significant differences in adverse effects [117].

Adverse Events and Potential Drug–Drug Interaction Risks

The oral NK1-receptor antagonists are generally very well tolerated with no obvious differences in adverse event profiles. The most commonly described adverse events are headache, constipation, and hiccups, but in some of the pivotal trials these adverse events were not different in frequency or intensity compared with the placebo-control arms. Fosaprepitant (intravenous prodrug of aprepitant) has some local hypersensitivity reactions, in particular in AC patients, which is probably due to surfactant PS 80 [118]. HTX-019 (intravenous aprepitant) without surfactant has a lower incidence of hypersensitivity reactions [119] as does intravenous NEPA [118]. Intravenous rolapitant is no longer available due to a number of anaphylactic reactions.

Potential drug–drug interaction risks have been very well investigated and described for the NK1-receptor antagonists. The major difference is that aprepitant and netupitant are primarily metabolized through CYP3A4, whereas rolapitant is primarily metabolized through CYP2D6. This results in a difference in potential drug–drug interaction risks. For example, although it is recommended that the dose of dexamethasone is reduced to approximately 50% when combined with aprepitant or netupitant, this is not necessary when used together with rolapitant. For an overview of potential drug–drug interaction risks, see Table 7.

Table 7

Potential drug–drug interaction risks with the NK1-receptor antagonists aprepitant, netupitant, and rolapitant

	Aprepitant	Netupitant	Rolapitant
CYP enzymes	3A4, 1A2, 2C9	3A4	2D6
Mechanism	Inhibitor of 3A4 and substrate for 3A4 and inducer of 3A4 and 2C9	Inhibitor of 3A4 and substrate for 3A4	Inhibitor of 2D6 and of BCRP
No DI risk	IV vinorelbine, docetaxel, cyclophosphamide, ondansetron, granisetron, palonosetron, digoxin	Palonosetron, digoxin, docetaxel, etoposide, cyclophosphamide, digoxin	Dexamethasone, ranitidine, ondansetron, metoclopramide, doxorubicin, epirubicin, irinotecan, topotecan, docetaxel, 5-FU, etoposide, methotrexate, ketoconazole, midazolam
PDI risks	Dexamethasone, methylprednisolone, warfarin, oral contraceptives, midazolam, tolbutamid, ifosfamide, ritonavir clarithromycin, itraconazole, phenytoin rifampicin, phenobarbital, carbamazepine, oxycodone	Dexamethasone, methylprednisolone, oral contraceptives, clarithromycin, erythromycin, itraconazole, ritonavir, rifampicin, carbamazepine, phenytoin, phenobarbital, SSRI, SNRI	Antidepressants, thioridazine, pimozide

BCRP breast cancer resistance protein, CYP cytochrome 450, DI drug–drug interaction, IV intravenously, PDI potential drug–drug interaction, SNRI selective noradrenaline reuptake inhibitor, SSRI selective serotonin reuptake inhibitor

Bold indicates the primary metabolizing CYP enzyme for each antiemetic agent

Others

Cannabinoids

The cannabinoid delta-9-tetrahydrocannabinol (Δ-9-THC) and the synthetic cannabinoids dronabinol and nabilone were investigated in a number of trials in the 1970s and 1980s. Only a few randomized trials with small sample sizes were conducted and the majority did not comply with today’s recommended trial methodology. Furthermore, adverse events such as dysphoria, euphoria, dizziness, and sedation were frequent making use difficult in older patients with cancer. These trials all used cannabinol and compared the cannabinol with antiemetics such as prochlorperazine and other dopamine-receptor antagonists no longer recommended as standard antiemetic therapy.

Meiri and coworkers compared the antiemetic effect of dronabinol, ondansetron, and the combination with placebo in patients receiving moderate- or high-emetic-risk chemotherapy (n = 61). Unfortunately, the study was prematurely closed and no relevant conclusions can be drawn [120].

A recent phase II, randomized, double-blind, placebo-controlled, crossover study (n = 72) investigated the antiemetic effect of an extract of THC and cannabidiol (CBD) in patients with refractory chemotherapy-induced nausea and/or vomiting [121]. The authors concluded that the addition THC/CBD to standard antiemetics resulted in less nausea and vomiting but also in additional adverse events. The median age of patients in this trial was only 55 years, meaning that more adverse events could be expected in real-life patients with cancer who are 10–15 years older. Due to the modest antiemetic effect and the high risk of adverse effects, interest in investigating cannabinoids in combination with modern antiemetics has been limited. The National Comprehensive Cancer Network (NCCN) antiemetic guidelines include dronabinol as an antiemetic in breakthrough nausea and vomiting not responding to other antiemetics, but no other evidence-based guidelines recommend the use of cannabinoids for CINV [5], and a recent systematic review concluded that although there is some neurophysiological support for the use of cannabinoids in CINV, this is not supported by randomized clinical trials [122].

Olanzapine

Olanzapine is approved as an antipsychotic drug targeting multiple receptors such as D1–D4, 5-HT2A, 5-HT2C, 5-HT3, 5-HT6, histamine H1, α1-adrenergic, acetylcholine, and muscarinic receptors [123] and has been investigated as an antiemetic in a number of phase II [124-127] and phase III trials [128-130] and addressed in a number of scientific reviews [131, 132].

In an open-designed, phase III study (n = 241), chemotherapy-naïve patients were treated with cisplatin-based (≥ 70 mg/m2) or AC chemotherapy and all received palonosetron plus dexamethasone as antiemetic prophylaxis on day 1. Patients were randomized to receive either olanzapine 10 mg once daily on days 1–4 (OPD) or aprepitant on days 1–3 plus dexamethasone on days 2–4 (APD) as additional antiemetic prophylaxis. No significant difference was found in CR (no emesis and no rescue antiemetics 0–120 h after initiation of chemotherapy), but nausea was better controlled with the OPD regimen [128].

A randomized, double-blind study (n = 380) in chemotherapy-naïve patients receiving cisplatin-based (≥ 70 mg/m2) or AC chemotherapy compared olanzapine (10 mg × 1 orally on days 1–4) with placebo, both in combination with aprepitant (or fosaprepitant) plus a 5-HT3-receptor antagonist plus dexamethasone [129]. Nausea prevention (the primary endpoint) was significantly improved by olanzapine, as were the CR rates (no emesis and no rescue antiemetics) 0–24 h, 25–120 h and 0–120 h after initiation of chemotherapy, respectively [129]. Some patients had increased sedation with olanzapine, which was severe in 5%. Again, the median age in this trial was only 57 years (approximately 10 years younger than real-life patients), meaning that the risk of sedation could be higher in older real-life patients.

A recent, randomized, double-blind trial (n = 710) in chemotherapy-naïve patients treated with cisplatin-based chemotherapy (≥ 50 mg/m2) demonstrated that a 5-mg dose of olanzapine (once daily on days 1–4) is also superior to placebo (both combined with aprepitant, palonosetron and dexamethasone) [130].

Based on these three trials, olanzapine is now recommended as an option in evidence-based antiemetic guidelines [5]. Besides sedation, postural hypotension, fatigue, and anticholinergic effects have been described.

Evidence-Based Prophylaxis of Chemotherapy-Induced Nausea and Vomiting

Several guidelines have been published, but the most frequently used are the Multinational Association of Supportive Care in Cancer/European Society for Medical Oncology (MASCC/ESMO) [133, 134], the American Society of Clinical Oncology (ASCO) [135], and the NCCN [136] guidelines. The MASCC/ESMO and ASCO guidelines are strictly evidence-based, whereas the NCCN guidelines are more pragmatic based on evidence but also on experts’ opinion. There are only minor differences between the guideline recommendations; primarily, the NCCN guidelines have more detailed recommendations and a more extended indication for some antiemetics than the others. The MASCC/ESMO and ASCO guidelines are updated when new data have been published. The NCCN guidelines are updated once every year. None of the guidelines have specific recommendations for older patients receiving chemotherapy, although the NCCN guidelines do have some pharmacological considerations.

Guidelines provide recommendations for the prophylaxis of acute and delayed emesis induced by single-day chemotherapy and multiple-day chemotherapy. Recommendations are also provided for breakthrough nausea and vomiting and for anticipatory nausea and vomiting. Recommendations are given for both adult and pediatric patients. Below is a summary (adults only) of the recommendations for the prophylaxis of acute and delayed CINV induced by single-day IV chemotherapy or by multiple-day IV chemotherapy with moderate- and/or high-emetic-risk IV chemotherapy on day 1 only.

Minimal Emetic Risk (< 10%)

None of the guidelines recommended routine antiemetic prophylaxis. Patients should have access to rescue antiemetics such as a D2-receptor antagonist, a 5-HT3-receptor antagonist or a corticosteroid.

Low Emetic Risk (10–30%)

A dopamine-receptor antagonist (MASCC/ESMO, NCCN), a serotonin-receptor antagonist (MASCC/ESMO, ASCO, NCCN) or dexamethasone (MASCC/ESMO, ASCO, NCCN) is recommended for prophylaxis in the first 24 h after chemotherapy. None of the guidelines recommend routine antiemetics for delayed CINV protection.

Moderate Emetic Risk (30–90%)

Carboplatin

Patients treated with carboplatin ≥ AUC 4 mg/mL/min are recommended a three-drug combination of an NK1-receptor antagonist, a 5-HT3-receptor antagonist, and dexamethasone (day 1). The NCCN guidelines consider carboplatin a drug with high emetic risk, although the risk of emesis in the first 24 h after carboplatin is < 90% [137]. In patients receiving the above three-drug combination only, rescue antiemetics are recommended after the first 24 h.

Other than Carboplatin

Patients treated with moderate-emetic-risk chemotherapy other than carboplatin ≥4 mg/mL/min are recommended a two-drug combination of a 5-HT3-receptor antagonist and dexamethasone on day 1 (MASCC/ESMO, ASCO, NCCN). Patients treated with cyclophosphamide, doxorubicin/epirubicin, or oxaliplatin (MASCC/ESMO, ASCO, NCCN) and other moderate-emetic-risk agents known to cause delayed nausea and vomiting (ASCO, NCCN) may be offered dexamethasone on days 2–3. The NCCN guidelines also suggest an NK1-receptor antagonist or olanzapine (both as part of a three-drug regimen with a 5-HT3-receptor antagonist and dexamethasone) as an option on day 1 and as a single agent on days 2–3.

High Emetic Risk (> 90%)

The ASCO guidelines recommend a four-drug regimen of an NK1-receptor antagonist, a 5-HT3-receptor antagonist, dexamethasone, and olanzapine for prophylaxis of CINV induced by a single agent (cisplatin and other) high-emetic-risk chemotherapy or induced by the AC combination (day 1). It is recommended to continue dexamethasone and olanzapine on days 2–4 in cisplatin-based chemotherapy and to continue olanzapine on days 2–4 in AC chemotherapy. If the NK1-receptor antagonist chosen is aprepitant, aprepitant should be continued on days 2–3. Both MASCC and NCCN recommend the four-drug regimen as well, but also suggest two different three-drug regimens as alternative options (palonosetron and dexamethasone combined with olanzapine [day 1] or a 5-HT3-receptor antagonist and dexamethasone combined with an NK1-receptor antagonist [day 1], with the same treatment on days 2–4 or days 2–3 as described above).

Conclusion and Future Perspectives

Evidence-based recommendations for the prophylaxis of CINV have been optimized during the past 40 years. Today, vomiting can be prevented in the majority of patients, whereas nausea remains a significant problem. This is due to the fact that 5-HT3-receptor antagonists and NK1-receptor antagonists are very effective in the prophylaxis of emesis, but only have limited effect against nausea. The most effective anti-nausea agents seem to be those targeting multiple receptors, such as olanzapine.

None of the guidelines have specific recommendations for older patients receiving chemotherapy. Young age is a risk factor for CINV, meaning that older patients have a lower risk of CINV than younger patients provided they receive the same kind of chemotherapy and antiemetic prophylaxis. Our knowledge about the risk of CINV in older patients is limited, because randomized clinical trials (RCTs) do not represent real-life patients. Patients included in RCTs are younger, they have less comorbidity and use a lower number of medications than real-life patients. In a review of >260,000 patients included in 302 trials published on the ClinicalTrials.gov website in the period 1994–2015, the average age of included patients was almost 7 years younger than the average age of the background cancer population in the same period [138]. The average number of exclusion criteria in industry-sponsored trials is 49 [139] and 91% of trials have exclusion criteria with respect to physical function and 85% with respect to organ function [140]. This is also a fact as concerns RCTs in CINV.

In Table 8, median or mean age is listed for patients included in the pivotal and largest post-marketing studies of 5-HT3-receptor antagonists and NK1-receptor antagonists (see also Tables 1, 2, 3, 4, 5 and 6). In all but two of the 21 trials with data of median (or mean) age, the median (mean) age is < 60 years. As in other RCTs, this is 5–10 years younger than in real-life patients. Because of the younger age of patients in CINV RCTs as compared with real-life patients, one could speculate that the emetic risk of chemotherapy in the RCTs is higher than in real-life. Therefore, some older patients may have been over treated with antiemetics.

Table 8

Age of patients included in industry-funded pivotal trials and largest post-marketing studies in Tables 1, 2, 3, 4, 5 and 6

References	Age, years; median or mean (range)
	Investigational arm	Standard/placebo arm
Marty et al. [78]	Median 57 (29–69)	Median 57 (29–69)
Bonneterre et al. [79]	No data	No data
Kaasa et al. [80]	Median 58 (19–80)	Median 58 (19–80)
Marschner et al. [81]	Median 55 (28–79)	Median 53 (29–77)
Warr et al. [84]	Median 57 (no data)	Median 55 (no data)
Perez et al. [85]	Mean 55 (18–87)	Mean 56 (21–94)
Gralla et al. [86]	Mean 62 (19–87)	Mean 62 (20–88)
Gralla et al. [88]	Mean 56 (no data)	Mean 55 (no data)
Eisenberg et al. [89]	Mean 53 (no data)	Mean 54 (no data)
Aapro et al. [90]	Mean 53 (no data)	Mean 51 (no data)
Saito et al. [91]	Mean 58 (no data)	Mean 58 (no data)
Navari et al. [97]	Mean 64 (no data)	Mean 60 (no data)
Chawla et al. [101]	Mean 56 (no data)	Mean 54 (no data)
Hesketh et al. [102]	Mean 59 (no data)	Mean 58 (no data)
Poli-Bigelli et al. [103]	Mean 54 (no data)	Mean 53 (no data)
Warr et al. [105]	Mean 53 (no data)	Mean 52 (no data)
Hesketh et al. [109]	Median 53 (19–77)	Median 55 (no data)
Aapro et al. [110]	Median 54 (22–79)	Median 54 (no data)
Gralla et al. [112]	Median 57 (27–76)	Median 59 (no data)
Rapoport et al. [115]	Median 56 (20–75)	Median 54 (18–77)
Rapoport et al. [116]	Median 59 (21–86)	Median 59 (18–90)
Schwartzberg et al. [117]	Median 58 (22–86)	Median 56 (22–88)

As previously mentioned, a number of studies have investigated steroid-sparing regimens comparing dexamethasone on day 1 of chemotherapy only with 2–4 days of dexamethasone [141, 142]. With cisplatin-based chemotherapy as an exception, it seems that dexamethasone on day 1 is as good as several days of dexamethasone. In cisplatin-based chemotherapy, no clear-cut conclusion can be drawn from studies currently available [143, 144]. In patients receiving immunotherapy, the lowest effective dose of dexamethasone is recommended [145] and the lowest effective dose is also recommended for prophylaxis of CINV during the COVID-19 pandemic [146]. This is of special interest for older cancer patients, because the single-day dexamethasone strategy enables the entire antiemetic prophylaxis to be administered before chemotherapy with no need for routine antiemetics in the subsequent days, resulting in optimal compliance. For example, for the prophylaxis of carboplatin-induced nausea and vomiting, guidelines recommend the combination of single doses of a 5-HT3-receptor antagonist, dexamethasone, and one of the long-acting NK1-receptor antagonists (netupitant or rolapitant) as an option [133].

Also, when using olanzapine for prophylaxis of CINV in older cancer patients, the lowest effective dose should be used. Studies confirm that olanzapine 5 mg is superior to placebo [130], but no large RCT has directly compared 5 mg and 10 mg of olanzapine. In older patients, it seems reasonable to start with the 5-mg dose of olanzapine to avoid the risk of severe sedation.

Other considerations should be taken into account when prescribing antiemetics to older patients with cancer. Figure 1 shows a flow diagram with these considerations and recommendations for prescribing antiemetics to older patients.

Fig. 1

Flow diagram for prescribing antiemetic prophylaxis of CINV in older cancer patients

Future trials should investigate deprescription of antiemetics in older patients in order to reduce the risk of drug–drug interactions and to reduce costs. A meta-analysis of four previously published studies concluded that the NK1-receptor antagonist, aprepitant, increased the antiemetic effect of a 5-HT3-receptor antagonist plus dexamethasone in patients aged 65 + years as compared with placebo, but in fact this difference was only statistically significant in one of the four trials [147]. Another post-hoc subanalysis of three previously published trials concluded that NEPA is effective and well tolerated in older patients receiving moderately or highly emetogenic chemotherapy [148]. Since our knowledge of the use of NK1-receptor antagonists in older cancer patients is limited to post-hoc subanalysis of previously published studies, we need a well-designed prospective phase II trial that limits inclusion to older patients with cancer (e.g., 70 + years old) receiving emetogenic chemotherapy and investigates deprescription of antiemetics (two antiemetics instead of three) and includes a preplanned subanalysis of patients with other emetogenic low risk factors (e.g., men vs women). In case of promising phase II results, a phase III RCT should follow comparing two versus three antiemetics in a double-blind noninferiority design. If non-inferiority (of two antiemetics versus three) is confirmed, guidelines should be updated accordingly including specific recommendations for older patients.

Older patients have a lower risk for chemotherapy-induced nausea and vomiting (CINV) than younger ones.

Evidence-based CINV guidelines do not include specific recommendations for older patients with cancer.

This review summarizes the evidence for prophylaxis of CINV focusing on older patients with cancer.