Adverse Drug Reaction Classification System

Pharmaceutical Information
Drug Name Dexlansoprazole
Drug ID BADD_D00628
Description Dexlansoprazole is a new generation proton pump inhibitor (PPI) used for the management of symptoms associated with gastroesophageal reflux disease (GERD) and erosive esophagitis. Dexlansoprazole is the R-enantiomer of [DB00448], which is composed of a racemic mixture of the R- and S-enantiomers. Compared to the older generation of PPIs (which includes [DB00213], [DB00338], and [DB00448]) [A178084], dexlansoprazole MR has a unique pharmacokinetic profile due to its delayed-release and dual-delivery release system. The active ingredient is released in two phases at different pH values and at different time points, resulting in two peak concentrations in the blood; 25% of the dose is released at pH 5.5 in the proximal duodenum, while the remaining 75% is released at pH 6.75 in the distal small intestine [A19567]. As a result, dexlansoprazole has a peak concentration within 1-2 hours after dosing and another within 4-5 hours [FDA Label]. Dexlansoprazole's unique pharmacokinetics addresses limitations of the older generation PPIs including short plasma half-life, break-through symptoms, and need for meal-associated dosing [A19568]. These characteristics make dexlansoprazole a good option for people who struggle with adherence and strict dosage timing before meals[A178087, A19566]. Dexlansoprazole exerts its stomach acid-suppressing effects in the same way as other drugs in the PPI family by inhibiting the final step in gastric acid production. Dexlansoprazole targets the (H+, K+)-ATPase enzyme, which is involved in the secretion of hydrochloric acid through the exchange of H+ ions from the cytoplasm for K+ ions. Normally functioning (H+, K+)-ATPase stimulates hydrochloric acid secretion into the gastric lumen thereby increasing stomach acidity and lowering pH. Once absorbed into circulation, dexlansoprazole covalently binds to the sulfhydryl groups of cysteines found on the (H+, K+)-ATPase enzyme at the secretory surface of gastric parietal cells, which leads to inhibition of both basal and stimulated gastric acid secretion. Despite dexlansoprazole's unique pharmacokinetic profile, efficacy in management of GERD symptoms is considered similar to other medications within the PPI class including [DB00338], [DB00736], [DB00448], [DB00213], and [DB01129]. Due to their good safety profile and as several PPIs are available over the counter without a prescription, their current use in North America is widespread. Long term use of PPIs such as dexlansoprazole have been associated with possible adverse effects, however, including increased susceptibility to bacterial infections (including gastrointestinal _C. difficile_), reduced absorption of micronutrients including iron and B12, and an increased risk of developing hypomagnesemia and hypocalcemia which may contribute to osteoporosis and bone fractures later in life [A177571]. PPIs such as dexlansoprazole have also been shown to inhibit the activity of dimethylarginine dimethylaminohydrolase (DDAH), an enzyme necessary for cardiovascular health. DDAH inhibition causes a consequent accumulation of the nitric oxide synthase inhibitor asymmetric dimethylarginine (ADMA), which is thought to cause the association of PPIs with increased risk of cardiovascular events in patients with unstable coronary syndromes [A177577, A177580]. Dexlansoprazole doses should be slowly lowered, or tapered, before discontinuing as rapid discontinuation of PPIs such as dexlansoprazole may cause a rebound effect and a short term increase in hypersecretion [A177574].
Indications and Usage Dexlansoprazole is indicated for healing all grades of erosive esophagitis (EE), maintaining and healing of EE and relief of heartburn, and treating heartburn associated with symptomatic non-erosive gastroesophageal reflux disease (GERD).
Marketing Status approved; investigational
ATC Code A02BC06
DrugBank ID DB05351
KEGG ID D08903
MeSH ID D064748
PubChem ID 9578005
TTD Drug ID D06YYD
NDC Product Code 47234-1148; 24979-704; 49884-147; 55154-5154; 64764-171; 42765-012; 55111-905; 70518-3693; 49884-148; 51407-747; 49711-1513; 65372-1182; 65977-0118; 24979-703; 50090-5944; 11532-1148; 24979-001; 24979-002; 47234-1147; 50090-6514; 64764-175; 14501-0057; 55111-909; 65977-0141; 66005-0031; 51407-746; 11532-1147; 59285-038
UNII UYE4T5I70X
Synonyms Dexlansoprazole | Lansoprazole, R-Isomer | Lansoprazole, R Isomer | R-Isomer Lansoprazole | 2-((R)-((3-Methyl-4-(2,2,2-trifluoroethoxy)-2-pyridinyl)methyl)sulfinyl)-1H-benzimidazole | R-Lansoprazole | R Lansoprazole | Dexlansoprazole Sesquihydrate | TAK 390MR | TAK390MR | TAK-390MR | TAK-390 | TAK 390 | TAK390 | Dexilant | T-168390 | T 168390 | T168390
Chemical Information
Molecular Formula C16H14F3N3O2S
CAS Registry Number 138530-94-6
SMILES CC1=C(C=CN=C1CS(=O)C2=NC3=CC=CC=C3N2)OCC(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)
Vision blurred17.17.01.010; 06.02.06.0070.000747%
Visual impairment06.02.10.0130.000304%Not Available
Vomiting07.01.07.0030.002102%
Vulvovaginitis21.14.02.005; 11.01.10.003--Not Available
Weight increased13.15.01.006--
Wheezing22.03.01.0090.000138%
Withdrawal syndrome19.07.06.023; 08.06.02.0120.000470%Not Available
Tubulointerstitial nephritis20.05.02.0020.000138%Not Available
Hypoacusis04.02.01.0060.000138%
Peripheral swelling08.01.03.053; 02.05.04.0150.000608%Not Available
Osteopenia15.02.03.003; 14.04.04.0040.000470%Not Available
Blood bilirubin decreased13.03.04.017--Not Available
Deep vein thrombosis24.01.02.003--Not Available
Dyschezia07.02.03.005--Not Available
Large intestine polyp07.20.01.010; 16.05.02.006--Not Available
Acute coronary syndrome24.04.04.011; 02.02.02.015--Not Available
Respiratory tract congestion22.02.07.003--Not Available
Lymphatic disorder01.09.01.003--Not Available
Gastrointestinal hypermotility07.02.04.005--Not Available
Musculoskeletal stiffness15.03.05.027--Not Available
Musculoskeletal discomfort15.03.04.001--Not Available
Nodule08.03.05.002--Not Available
Varices oesophageal24.10.02.004; 09.01.06.009; 07.15.05.0010.000138%Not Available
Colitis microscopic07.08.01.011--Not Available
Rectal tenesmus15.05.03.011; 07.03.03.001--Not Available
Paraesthesia oral07.05.05.035; 17.02.06.0080.000207%Not Available
Restless legs syndrome17.02.07.008; 15.05.03.012--Not Available
Angiopathy24.03.02.007--Not Available
Blood alkaline phosphatase increased13.04.02.004--
Hot flush24.03.01.005; 21.02.02.001; 08.01.03.0270.000207%
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