ADReCS

Pharmaceutical Information

Drug Name	Apalutamide
Drug ID	BADD_D02490
Description	Apalutamide is a potent androgen receptor (AR) antagonist that selectively binds to the ligand-binding domain of AR and blocks AR nuclear translocation or binding to androgen response elements [A31846]. It has been used in trials studying the treatment of Prostate Cancer, Hepatic Impairment, Prostatic Neoplasms, Castration-Resistant Prostate Cancer, and Prostatic Neoplasms, Castration-Resistant, among others. Exerting an antitumor action, apalutamide blocking the effect of androgens that promote tumor growth. It targets the AR ligand-binding domain and prevents AR nuclear translocation, DNA binding, and transcription of AR gene targets in prostate tumors [A31846]. In mice bearing human CRPC xenograft models, apalutamide treatment produced tumor regressions in a dose-dependent manner that was more effective than that of [DB01128] or [DB08899]. Unlike bicalutamide, apalutamide antagonized AR-mediated signaling in AR overexpressing human CRPC cell lines [A31846]. Androgen-deprivation therapy, or hormone therapy, can be used as part of maintenance therapy for patients with non-metastatic prostate cancer. Although most patients achieve therapeutic responses at the initial hormone therapy, many patients progress to non-metastatic castration-resistant (resistance to hormone therapy) prostate cancer which is the second-most common cause of cancer-related deaths in American males [A31852]. Castration-resistant prostate cancer is often incurable, which poses significant clinical challenges for patients. Approximately 10 to 20 % of prostate cancer cases are castration-resistant, and up to 16% of these patients show no evidence of cancer metastasis at the time of castration-resistant diagnosis [L1295]. Higher prostate-specific antigen (PSA) and shorter PSA doubling time (PSA DT) are associated with a higher risk for metastases and death [A31846]. In a phase-2 multicenter open-label study, 89% of patients with non-metastatic, castration-resistant prostate cancer had ≥50% PSA decline at week 12 of apalutamide treatment [A31846]. In a randomized trial, the median metastasis-free survival for patients taking apalutamide was 40.5 months compared to 16.2 months for patients taking a placebo [L1295]. Apalutamide displayed good tolerability and safety profile in clinical studies. Apalutamide was approved in February 2018 by the FDA as Erleada for the treatment of patients with non-metastatic prostate cancer that is resistant to treatment with hormone therapy (castration-resistant). It is available as oral tablets. Apalutamide is the first FDA-approved treatment for non-metastatic, castration-resistant prostate cancer [L1295].
Indications and Usage	Indicated for the treatment of patients with non-metastatic, castration-resistant prostate cancer (NM-CRPC) [FDA Label].
Marketing Status	approved; investigational
ATC Code	L02BB05
DrugBank ID	DB11901
KEGG ID	D11040
MeSH ID	C572045
PubChem ID	24872560
TTD Drug ID	D0S7LG
NDC Product Code	11014-0330; 59676-604; 59676-600; 68554-0127; 71796-033; 12578-621; 54893-0100; 71796-019; 65267-116; 11014-0485; 17314-215
UNII	4T36H88UA7
Synonyms	apalutamide \| ARN-509 \| Erleada

Chemical Information

Molecular Formula	C21H15F4N5O2S
CAS Registry Number	956104-40-8
SMILES	CNC(=O)C1=C(C=C(C=C1)N2C(=S)N(C(=O)C23CCC3)C4=CC(=C(N=C4)C#N)C(F)(F)F)F
Chemical Structure

ADRs Induced by Drug

*The priority for ADR severity classification is based on FAERS assessment, followed by the most severe level in CTCAE rating. If neither is available, it will be displayed as 'Not available'.
**The 'Not Available' level is hidden by default and can be restored by clicking on the legend twice.

ADR Term	ADReCS ID	ADR Frequency (FAERS)	ADR Severity Grade (FAERS)	ADR Severity Grade (CTCAE)
Abnormal dreams	17.15.02.001; 19.02.03.001	0.001702%		-
Ageusia	07.14.03.003; 17.02.07.001	0.002035%		-
Agranulocytosis	01.02.03.001	0.001335%		-
Altered state of consciousness	17.02.04.001; 19.07.01.003	0.000501%		-
Angina pectoris	02.02.02.002; 24.04.04.002	0.001001%
Aortic aneurysm rupture	24.02.03.003	0.000334%		-
Aortic dissection	24.02.03.002	0.000334%		-
Aortic stenosis	24.04.01.001	0.000334%		-
Aphasia	17.02.03.001; 19.21.01.001	0.000901%
Aphonia	17.02.08.009; 19.19.01.002; 22.12.03.001	0.000734%
Arthralgia	15.01.02.001	0.016917%
Asthenia	08.01.01.001	0.014815%		-
Atrial fibrillation	02.03.03.002	0.003003%
Back pain	15.03.04.005	-	-
Blister	12.01.06.002; 23.03.01.001	0.001235%		-
Bone pain	15.02.01.001	0.002436%
Breast tenderness	21.05.05.004	0.001135%		-
Bronchiectasis	22.03.02.005	0.000334%		-
Cardiac failure	02.05.01.001	0.002503%
Cardiovascular disorder	02.11.01.010; 24.03.02.009	0.000901%		-
Cerebral haemorrhage	17.08.01.003; 24.07.04.001	0.001168%		-
Cerebral infarction	17.08.01.004; 24.04.06.002	0.001168%		-
Cerebral ischaemia	17.08.01.005; 24.04.06.003	0.000501%
Cerebrovascular accident	17.08.01.007; 24.03.05.001	-	-
Choking	22.12.03.003	0.000501%		-
Cold sweat	08.01.03.024; 23.02.03.002	0.000734%		-
Colon cancer	07.21.01.001; 16.13.01.001	0.000334%		-
Confusional state	17.02.03.005; 19.13.01.001	-	-
Constipation	07.02.02.001	-	-
Coronary artery disease	02.02.01.001; 24.04.04.006	0.000334%		-

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