Adverse Drug Reaction Classification System

Pharmaceutical Information
Drug Name Rucaparib
Drug ID BADD_D02510
Description Rucaparib is a potent mammalian poly(ADP-ribose) polymerase (PARP) 1, 2 and 3 inhibitor with anticancer properties. PPAR is an enzyme that plays an essential role in DNA repair by activating response pathways and facilitating repair [A18745], and defects in these repair mechanisms have been demonstrated in various malignancies, including cancer. Regulation of repair pathways is critical in promoting necessary cell death. BRCA genes are tumor suppressor genes mediate several cellular process including DNA replication, transcription regulation, cell cycle checkpoints, apoptosis, chromatin structuring and homologous recombination (HR). Homologous recombination deficiency (HRD), along with PPAR inhibition, is a vulnerability that enhances the cell death pathway when the single mutations alone would permit viability. Ovarian cancer commonly possesses defects in DNA repair pathways such as HRD due to BRCA mutations or otherwise. There are three main types of ovarian cancer: epithelial (90%), germ cell (5%) and sex cord stromal cell (5%). Epithelial ovarian, being the most common, fifth leading cause of cancer-related deaths in women in the United States. Advanced ovarian cancer particularly poses challenges due to reduced therapeutic response rates from standard platinum-based chemotherapy and overall survival rates. Rucaparib has shown to induce cytotoxicity in tumor cell lines with deficiencies in BRCA1/2 and other DNA repair genes [FDA Label]. Of all the BRCA1/2 mutations in ovarian cancer, most are due to germline mutations (18%), and approximately 7% represent somatic mutations acquired within the tumor [A31354]. The indication of rucaparib as an oral monotherapy in patients with deleterious BRCA mutation (germline and/or somatic) associated advanced ovarian cancer was granted accelerated approval in 2016 for selected patients who have previously received greater than two lines of platinum-based therapy. It is currently marketed in the US under the brand name Rubraca that contains rucaparib camsylate as the active ingredient. The identification of patients who are eligible for rucaparib therapy is performed via *in vitro* diagnostic tests to detect the presence of a deleterious BRCA mutation (germline and/or somatic). The FDA-approved test qualitatively detects sequence alterations in BRCA1 and BRCA2 (BRCA1/2) genes. More information can be found on the FDA Website [L1047]. While rucaparib is indicated for deleterious BRCA mutation (germline and/or somatic)-associated advanced ovarian cancer, there is evidence that its antitumor activity is also clinically effective against ovarian tumors with high homologous recombination deficiency (HRD) loss of heterozygosity (LOH) [A31354].
Indications and Usage Indicated as monotherapy for the treatment of patients with deleterious BRCA mutation (germline and/or somatic) associated advanced ovarian cancer who have been treated with two or more chemotherapies. Select patients for therapy based on an FDA-approved companion diagnostic for rucaparib.
Marketing Status approved; investigational
ATC Code L01XK03
DrugBank ID DB12332
KEGG ID D10079
MeSH ID C531549
PubChem ID 9931954
TTD Drug ID D01SHZ
NDC Product Code 69660-202; 69660-203; 69660-201
UNII 8237F3U7EH
Synonyms rucaparib | PF-01367338 | Rubraca | AG 014699 | AG014699 | AG-014699
Chemical Information
Molecular Formula C19H18FN3O
CAS Registry Number 283173-50-2
SMILES CNCC1=CC=C(C=C1)C2=C3CCNC(=O)C4=C3C(=CC(=C4)F)N2
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)
Hot flush24.03.01.005; 21.02.02.001; 08.01.03.0270.004186%
Abdominal neoplasm16.16.02.002; 07.21.04.0010.000280%Not Available
Adverse event08.06.01.0100.025934%Not Available
Appetite disorder19.09.01.002; 14.03.01.0040.000246%Not Available
Feeding disorder19.09.01.003; 14.03.02.0030.002597%Not Available
Gastrointestinal motility disorder07.02.03.0010.000985%Not Available
Haematotoxicity12.03.01.025; 01.05.01.0070.000437%Not Available
Limb discomfort15.03.04.0140.000795%Not Available
Malnutrition14.03.02.0040.000112%Not Available
Oesophageal disorder07.11.02.0010.000246%Not Available
Decreased appetite08.01.09.028; 14.03.01.0050.039623%
Feeling of body temperature change08.01.09.0120.000381%Not Available
Sensation of foreign body08.01.09.0020.000246%Not Available
Blood disorder01.05.01.0040.000795%Not Available
Immunodeficiency10.03.02.0020.000224%Not Available
Adverse drug reaction08.06.01.0090.004388%Not Available
Bone marrow disorder01.05.01.0060.000224%Not Available
Drug intolerance08.06.01.0130.011708%Not Available
Obstruction08.01.03.0230.000246%Not Available
Hepatic lesion09.01.08.0050.000492%Not Available
Large intestinal obstruction07.13.03.0030.000168%
Metastasis16.22.01.0010.000112%Not Available
Renal impairment20.01.03.0100.001567%Not Available
Sinus disorder22.04.06.0020.000683%
Unevaluable event08.01.03.0510.004074%Not Available
Poor quality sleep19.02.05.005; 17.15.04.0020.001063%Not Available
Increased upper airway secretion22.12.03.0070.000112%Not Available
Hypophagia19.09.01.004; 14.03.01.006; 07.01.06.0100.002059%Not Available
Skin haemorrhage24.07.01.103; 23.06.07.0010.000571%Not Available
Bone marrow failure01.03.03.0050.001175%
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