SPARTAN Trial: Efficacy of Apalutamide in Men with Nonmetastatic Castration-resistant Prostate Cancer

27 Nov, 23

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Introduction

Metastases are a significant complication of prostate cancer and a leading cause of death among men with the disease. Nearly all men who die from prostate cancer have antecedent metastases to bone or other sites, including the lymph nodes, lung, and liver.

Apalutamide is a nonsteroidal antiandrogen that binds directly to the ligand-binding domain of the androgen receptor and prevents androgen-receptor translocation, DNA binding, and androgen-receptor–mediated transcription agent.

Aim

SPARTAN (Selective Prostate Androgen Receptor Targeting with ARN-509) trial evaluated the efficacy of apalutamide in men with nonmetastatic castration-resistant prostate cancer who were at high risk for the development of metastasis

Patient Profile

Men with nonmetastatic castration-resistant prostate cancer and a prostate-specific antigen doubling time of 10 months or less

Table 1: Patient baseline characteristic

Characteristic	Apalutamide (N = 806)	Placebo (N = 401)
Age — yr.
Median	74	74
Range	48–94	52–97
Median time from initial diagnosis to randomization — yr	7.95	7.85
Prostate-specific antigen doubling time
Median — mo	4.40	4.50
≤6 Mo — no. (%)	576 (71.5)	284 (70.8)
>6 Mo — no. (%)	230 (28.5)	117 (29.2)
Use of bone-sparing agent — no. (%)
Yes	82 (10.2)	39 (9.7)
No	724 (89.8)	362 (90.3)
Classification of local or regional nodal disease — no. (%)
N0	673 (83.5)	336 (83.8)
N1	133 (16.5)	65 (16.2)
Previous prostate-cancer treatment — no. (%)
Prostatectomy or radiation therapy	617 (76.6)	307 (76.6)
Gonadotropin-releasing hormone analogue agonist	780 (96.8)	387 (96.5)
First-generation antiandrogen agent†	592 (73.4)	290 (72.3)

* There were no significant differences between groups in the demographic and disease characteristics at baseline.

† First-generation antiandrogen agents are flutamide, bicalutamide, and nilutamide.

Methods

Phase 3 trial Double-blind, placebo-controlled,
Patients were randomly assigned, in a 2:1 ratio, to receive apalutamide (240 mg per day) or placebo.
1207 men underwent randomization
- 806 to the apalutamide group
- 401 to the placebo group
All the patients continued to receive androgen-deprivation therapy

Endpoint

The primary end point was metastasis-free survival, which was defined as the time from randomization to the first detection of distant metastasis on imaging or death
The secondary end points were time to metastasis progression-free survival, time to symptomatic progression, overall survival, and time to the initiation of cytotoxic chemotherapy.

Results

Figure 1: Primary Endpoint: Metastasis-free survival with apalutamide vs Placebo

Secondary Endpoints

Time to symptomatic progression was significantly longer with apalutamide than with placebo (hazard ratio, 0.45; P<0.001)

Time to metastasis, progression-free survival, and time to symptomatic progression were significantly longer with apalutamide than with placebo (P<0.001 for all comparisons)

End Point	Apalutamide (N = 806)	Placebo (N = 401)	Hazard Ratio	P Value
Secondary end points (mo)
Median time to metastasis	40.5	16.6	0.27	<0.001
Median progression-free survival	40.5	14.7	0.29	<0.001
Median time to symptomatic progression	NR	NR	0.45	<0.001
Median overall survival	NR	39.0	0.70	0.07
Median time to the initiation of cytotoxic chemotherapy	NR	NR	0.44	—

Safety

The rate of adverse events leading to discontinuation of the trial regimen was 10.6% in the apalutamide group and 7.0% in the placebo group
The following adverse events occurred at a higher rate with apalutamide than with placebo: rash (23.8% vs. 5.5%), hypothyroidism (8.1% vs. 2.0%), and fracture (11.7% vs. 6.5%)

Table 2: Adverse event

Adverse Event*	Apalutamide (N = 803)		Placebo (N = 398)
	Any Grade	Grade 3 or 4	Any Grade	Grade 3 or 4
	no. of patients (%)
Any adverse event	775 (96.5)	362 (45.1)	371 (93.2)	136 (34.2)
Serious adverse event	199 (24.8)	—	92 (23.1)	—
Adverse event leading to discontinuation of the trial regimen	85 (10.6)	—	28 (7.0)	—
	85 (10.6)
Adverse event associated with death	10 (1.2)	—	1 (0.3)	—
Adverse events that occurred in ≥15% of patients in either group†
Fatigue^‡	244 (30.4)	7 (0.9)	84 (21.1)	1 (0.3)
Hypertension	199 (24.8)	115 (14.3)	79 (19.8)	47 (11.8)
Rash^‡	191 (23.8)	42 (5.2)	22 (5.5)	1 (0.3)
Diarrhea	163 (20.3)	8 (1.0)	60 (15.1)	2 (0.5)
Nausea	145 (18.1)	0	63 (15.8)	0
Weight loss	129 (16.1)	9 (1.1)	25 (6.3)	1 (0.3)
Arthralgia	128 (15.9)	0	30 (7.5)	0
Falls^‡	125 (15.6)	14 (1.7)	36 (9.0)	3 (0.8)
Other adverse events of interest
Fracture^‡	94 (11.7)	22 (2.7)	26 (6.5)	3 (0.8)
Dizziness	75 (9.3)	5 (0.6)	25 (6.3)	0
Hypothyroidism^‡	65 (8.1)	0	8 (2.0)	0
Mental-impairment disorder^§	41 (5.1)	0	12 (3.0)	0
Seizure^‡	2 (0.2)	0	0	0

* The incidences of the following adverse events in the apalutamide group versus the placebo group were adjusted for exposure (events per 100 patient-years): fatigue (incidence, 32.3 vs. 27.2), hypertension (36.3 vs. 38.7), rash (29.6 vs. 8.3), diarrhea (21.6 vs. 22.6), nausea (15.8 vs. 0.4), weight loss (18.3 vs. 10.5), arthralgia (14.7 vs. 8.0), falls (13.6 vs. 10.0), fracture (10.5 vs. 7.8), dizziness (7.7 vs. 6.6), hypothyroidism (7.6 vs. 2.2), mental-impairment disorder (3.9 vs. 3.4), and seizure (0.2 vs. 0).

† This category includes adverse events that occurred up to 28 days after the last dose of the trial regimen was administered.

‡ These adverse events were considered by the investigators to be related to the trial regimen.

§ Mental-impairment disorders included the following adverse events: disturbance in attention, memory impairment, cognitive disorder, and amnesia.

Conclusion

In men with nonmetastatic castration-resistant prostate cancer, metastasis free survival and time to symptomatic progression were significantly longer with apalutamide than with placebo.
Overall survival, time to the initiation of cytotoxic chemotherapy, and second progression– free survival was longer with apalutamide than with placebo

Reference

N Engl J Med 2018;378:1408-18.

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