Chloroquine

P01B - Antimalarials ATC P01BA01 Small molecule approved 1949 Oral Parenteral Natural product

JFDA label: Heroquine Syrup

Mechanism of Action

Binds to and inhibits DNA and RNA polymerase; interferes with metabolism and hemoglobin utilization by parasites; inhibits prostaglandin effects; chloroquine concentrates within parasite acid vesicles and raises internal pH resulting in inhibition of parasite growth; may involve aggregates of ferriprotoporphyrin IX acting as chloroquine receptors causing membrane damage; may also interfere with nucleoprotein synthesis

Indications

Approved

Extraintestinal amebiasis
Malaria

Off-label

Discoid lupus erythematosus

Antimicrobial Spectrum

Expected / intrinsic spectrum (EUCAST breakpoints & labels) — not local resistance. Source: openfda-label.

Protozoa

Organism	Activity	MIC
Entamoeba histolytica	Active	—
Plasmodium falciparum	Active	—
Plasmodium malariae	Active	—
Plasmodium ovale	Active	—
Plasmodium parasites	Active	—
Plasmodium vivax	Active	—

Contraindications

Source: Lexicomp

Hypersensitivity to chloroquine, 4-aminoquinoline compounds, or any component of the formulation Absolute
the presence of retinal or visual field changes of any etiology (when used for indications other than acute malaria) Absolute

Adverse Reactions

Very Common >10%Common 1–10%Uncommon 0.1–1% Rare 0.01–0.1%Very Rare <0.01%Not Known

Cardiac disorders (9)

Not Known Atrioventricular block · bundle branch block · cardiac arrhythmia · cardiomyopathy · ECG changes (including prolonged QRS and QTc intervals, T-wave inversion, or depression) · hypotension · torsades de pointes · ventricular fibrillation · ventricular tachycardia

Nervous system disorders (16)

Not Known Agitation · anxiety · confusion · decreased deep tendon reflex · delirium · depression · extrapyramidal reaction (dystonia, dyskinesia, protrusion of the tongue, torticollis) · hallucination · headache · insomnia · motor dysfunction (sensorimotor disorder) · personality changes · polyneuropathy · psychosis · seizure · suicidal tendencies

Hepatobiliary disorders (2)

Not Known Hepatitis · increased liver enzymes

Blood and lymphatic system disorders (6)

Not Known Agranulocytosis (reversible) · aplastic anemia · hemolytic anemia (in G6PD-deficient patients) · neutropenia · pancytopenia · thrombocytopenia

Immune system disorders (4)

Not Known Anaphylactoid reaction · anaphylaxis · angioedema · DRESS syndrome

Metabolism and nutrition disorders (1)

Not Known Hypoglycemia

Gastrointestinal disorders (5)

Not Known Abdominal cramps · anorexia · diarrhea · nausea · vomiting

Skin and subcutaneous tissue disorders (13)

Not Known Alopecia · bleaching of hair · blue gray skin pigmentation · erythema multiforme · exacerbation of psoriasis · exfoliative dermatitis · lichen planus · pleomorphic rash · pruritus · skin photosensitivity · Stevens-Johnson syndrome · toxic epidermal necrolysis · urticaria

Musculoskeletal and connective tissue disorders (3)

Not Known Myopathy · neuromuscular disease · proximal myopathy

Eye disorders (9)

Not Known Accommodation disturbances · blurred vision · corneal opacity (reversible) · macular degeneration (may be irreversible) · maculopathy (may be irreversible) · nocturnal amblyopia · retinopathy (including irreversible changes in some patients' long-term or high-dose therapy) · transient scotomata · visual field defects

Ear and labyrinth disorders (3)

Not Known Deafness (nerve) · hearing loss (risk increased in patients with preexisting auditory damage) · tinnitus

Dosing

Source: Lexicomp

Note: Each 250 mg of chloroquine phosphate is equivalent to 150 mg of chloroquine base Malaria chemoprophylaxis: Oral: 500 mg (300 mg base) weekly on the same day each week; begin 1 to 2 weeks prior to exposure; continue while in endemic area and for 4 weeks after leaving endemic area (CDC 2018) Malaria treatment, uncomplicated: Oral: 1 g (600 mg base) on day 1, followed by 500 mg (300 mg base) 6-, 24-, and 48 hours after first dose. Note: For treatment of chloroquine-sensitive P. vivax and P. ovale, concomitant therapy with an 8-aminoquinoline (eg, primaquine) is necessary (CDC 2013). Extraintestinal amebiasis: Oral: 1 g (600 mg base) daily for 2 days followed by 500 mg daily (300 mg base) for at least 2 to 3 weeks; may be combined with an intestinal amebicide. Lupus erythematosus (off-label use): Not considered first-line agent (Bezerra 2005; Lesiak 2008). Due to the risk of retinal toxicity, do not exceed a daily dose of 2.3 mg/kg/day of chloroquine phosphate using actual body weight; intermediate doses may be obtained by splitting tablets or eliminating a tablet on certain days of the week (AAO [Marmor 2016]).

(For additional information see "Chloroquine: Pediatric drug information") Note: Each 250 mg of chloroquine phosphate is equivalent to 150 mg of chloroquine base Malaria chemoprophylaxis: Oral: 8.3 mg/kg/week (5 mg/kg base) on the same day each week (not to exceed 500 mg/dose [300 mg base/dose]); begin 1 to 2 weeks prior to exposure; continue while in endemic area and for 4 weeks after leaving endemic area (CDC 2018) Malaria treatment, uncomplicated: Oral: 16.6 mg/kg (10 mg/kg base) on day 1 (maximum: 1,000 mg [600 mg base]), followed by 8.3 mg/kg (5 mg/kg base) (maximum: 500 mg [300 mg base]) 6-, 24-, and 48 hours after first dose (CDC 2013)

Refer to adult dosing.

There are no dosage adjustments provided in the manufacturer’s labeling; the following guidelines have been used by some clinicians (Aronoff 2007): GFR ≥10 mL/minute: No dosage adjustment necessary. GFR Hemodialysis, peritoneal dialysis: Administer 50% of dose. Continuous renal replacement therapy (CRRT): No dosage adjustment necessary.

There are no dosage adjustments provided in the manufacturer’s labeling; use with caution.

Warnings & Precautions

Source: Lexicomp

Cardiovascular effects

Cases of cardiomyopathy resulting in cardiac failure (sometimes fatal) have been reported during long term therapy at high doses. Monitor for signs and symptoms of cardiomyopathy; discontinue if cardiomyopathy develops. Consider chronic toxicity and discontinue chloroquine if conduction disorders (bundle branch block/AV block) are diagnosed. QT prolongation, torsade de pointes, and ventricular arrhythmias (some fatal) have been reported; risk is increased with high doses. Use with caution in patients with cardiac disease, history of ventricular arrhythmias, uncorrected hypokalemia and/or hypomagnesemia, or bradycardia, and during concomitant administration with QT interval prolonging agents due to potential for QT prolongation. In a scientific statement from the American Heart Association, chloroquine has been determined to be an agent that may either cause direct myocardial toxicity or exacerbate underlying myocardial dysfunction (magnitude: major) (AHA [Page 2016]).

Extrapyramidal effects

Acute extrapyramidal disorders may occur, usually resolving after discontinuation of therapy and/or symptomatic treatment.

Hematologic effects

Rare hematologic reactions including reversible agranulocytosis, aplastic anemia, neutropenia, pancytopenia, and thrombocytopenia have been reported; monitor CBC during prolonged therapy. Consider discontinuation if severe blood disorders occur that are unrelated to disease.

Hypoglycemia

Severe hypoglycemia, including loss of consciousness, has been reported in patients treated with or without antidiabetic agents. Counsel patients about risk of hypoglycemia and associated signs and symptoms.

Neuromuscular effects

Skeletal muscle myopathy or neuromyopathy, leading to progressive weakness and atrophy of proximal muscle groups have been reported; muscle strength (especially proximal muscles) should be assessed periodically during prolonged therapy; discontinue therapy if weakness occurs.

Retinal toxicity

Retinal toxicity, potentially causing irreversible retinopathy, is predominantly associated with high daily doses and a duration of >5 years of use of chloroquine or hydroxychloroquine in the treatment of rheumatic diseases. Other major risk factors include concurrent tamoxifen use, renal impairment, lower body weight, and potentially the presence of macular disease. Risk is most accurately assessed on the basis of duration of use relative to daily dose/body weight (Marmor [AAO 2016]; Melles 2014). Based on these risks, the American Academy of Ophthalmology (AAO) recommends not exceeding a daily chloroquine phosphate dosage of 2.3 mg/kg using actual body weight. Previous recommendations to use ideal body weight are no longer advised; very thin patients in particular were at increased risk for retinal toxicity using this practice. Current AAO guidelines do not specifically address dosing in obese patients. AAO also recommends baseline screening for retinal toxicity and annual screening beginning after 5 years of use (or sooner if major risk factors are present) (Marmor [AAO 2016]). Disease-related concerns:

Auditory damage

Use with caution in patients with preexisting auditory damage; discontinue immediately if hearing defects are noted.

G6PD deficiency

Although the manufacturer’s labeling recommends chloroquine be used with caution in patients with G6PD deficiency due to a potential for hemolytic anemia, there is limited data to support this risk. Many experts consider chloroquine, when given in usual therapeutic doses to WHO Class II and III G6PD deficient patients, to probably be safe (Cappellini 2008; Glader 2017; Luzzatto 2016; Youngster 2010). Safety in Class I G6PD deficiency (ie, severe form of the deficiency associated with chronic hemolytic anemia) is generally unknown (Glader 2017). In a trial conducted in West Africa involving 74 G6PD deficient patients (predominantly Class III deficiency), there were no cases of hemolysis reported following exposure to usual doses of chloroquine (Mandi 2005). In addition, the ACR Rheumatology guidelines do not mention the need to evaluate G6PD levels prior to initiation of therapy (Singh 2015).

Hepatic impairment

Use with caution in patients with hepatic impairment, alcoholism, or concurrent therapy with hepatotoxic agents.

Porphyria

Use with caution in patients with porphyria; may exacerbate disease symptoms.

Psoriasis

Use with caution in patients with psoriasis; may exacerbate disease symptoms.

Seizure disorder

Use with caution in patients with a history of seizure disorder; may cause seizures. Concurrent drug therapy issues:

Drug-drug interactions

Potentially significant interactions may exist, requiring dose or frequency adjustment, additional monitoring, and/or selection of alternative therapy. Consult drug interactions database for more detailed information. Other warnings/precautions:

Appropriate use

Chloroquine does not prevent relapses in patients with vivax or ovale malaria (not effective against exoerythrocytic forms); additional treatment with an antimalarial effective against these forms (eg, an 8-aminoquinoline) is required for the treatment of infections with P. vivax and P. ovale. Do not use for the treatment of complicated malaria (high-grade parasitemia and/or complications [eg, cerebral malaria, acute renal failure]).

Chloroquine resistance

Chloroquine is not effective against chloroquine- or hydroxychloroquine-resistant strains of Plasmodium species. Chloroquine resistance is widespread in P. falciparum and is reported in P. vivax. Prior to initiation of chloroquine for prophylaxis, it should be determined if chloroquine is appropriate for use in the region to be visited; do not use for malaria prophylaxis in areas where chloroquine resistance occurs. Patients should be treated with another antimalarial if patient is infected with a resistant strain of plasmodia.

Pregnancy & Lactation

Pregnancy

In animal reproduction studies, drug accumulated in fetal ocular tissues and remained for several months following drug elimination from the rest of the body. Chloroquine and its metabolites cross the placenta and can be detected in the cord blood and urine of the newborn infant (Akintonwa 1988; Essien 1982; Law 2008). In one study, chloroquine and its metabolites were measurable in the cord blood 89 days (mean) after the last maternal dose (Law 2008). Malaria infection in pregnant women may be more severe than in nonpregnant women and has a high risk of maternal and perinatal morbidity and mortality. Therefore, pregnant women and women who are likely to become pregnant are advised to avoid travel to malaria-risk areas. Chloroquine is recommended for the treatment of pregnant women for uncomplicated malaria in chloroquine-sensitive regions; when caused by chloroquine-sensitive P. vivax or P. ovale, pregnant women should be maintained on chloroquine prophylaxis for the duration of the

Lactation

Chloroquine and its metabolite can be detected in breast milk. Per product labeling, 11 lactating women with malaria were given a single oral dose of chloroquine 600 mg. The maximum daily dose to the breastfeeding infant was calculated to be 0.7% of the maternal dose. Additional information has been published and results are variable. In one study, the relative dose to the nursing infant was calculated to be 2.3% (chloroquine) and 1% (metabolite) of the weight-adjusted maternal dose with the sam

Monitoring

Clinical pearl	Evaluate neuromuscular function periodically during prolonged therapy. Periodic CBC in patients receiving prolonged therapy Ophthalmologic exam at baseline (fundus examination within the first year plus visual fields and spectral-domain optical coherence tomography [SD OCT] if maculopathy is present) to screen for retinal toxicity, followed by annual screening beginning after 5 years of use (or sooner if major risk factors are present) (Marmor [AAO 2016]).

Clinical pearl

Evaluate neuromuscular function periodically during prolonged therapy. Periodic CBC in patients receiving prolonged therapy Ophthalmologic exam at baseline (fundus examination within the first year plus visual fields and spectral-domain optical coherence tomography [SD OCT] if maculopathy is present) to screen for retinal toxicity, followed by annual screening beginning after 5 years of use (or sooner if major risk factors are present) (Marmor [AAO 2016]).

Chemistry & Properties

Formula	C18H26ClN3
Molecular weight	319.88 g/mol
IUPAC name	4-N-(7-chloroquinolin-4-yl)-1-N,1-N-diethylpentane-1,4-diamine
CAS	54-05-7
PubChem CID	2719
InChIKey	`WHTVZRBIWZFKQO-UHFFFAOYSA-N`
logP	4.81 (XLogP 4.6)
Polar surface area	28.16 Å²
H-bond acceptors / donors	3 / 1
Drug-likeness (QED)	0.76
Lipinski violations	0

SMILES

CCN(CC)CCCC(C)Nc1ccnc2cc(Cl)ccc12

Biology & Pharmacokinetics

Pharmacokinetics predicted

Bioavailability	10.0%
Half-life	0.561 h
Volume of distribution	11.91 L/kg
Protein binding	49.6%
BBB penetrant	Yes

Enzyme interactions

Enzyme	Role	Detail
CYP2B6	Inhibitor	—
CYP2C19	Substrate	—
CYP3A4	Substrate	—

Receptor binding (top 7)

Target	Action	Affinity
Cholinergic, muscarinic M5 (CHRM5)	Binding	pKi 9.4
Norepinephrine transporter	Binding	pKi 6.0
5-HT1A (HTR1A)	Binding	pKi 5.2
5-HT2C (HTR2C)	Binding	pKi 5.2
5-HT2A (HTR2A)	Binding	pKi 5.2
DAT	Binding	pKi 5.1
SERT	Binding	pKi 5.1

Transporters

ASBT (Inhibitor)BCRP (Inhibitor)BCRP (Inhibitor)BSEP (Inhibitor)BSEP (Inhibitor)MATE1 (Inhibitor)MATE2 (Inhibitor)MDR1 (Inhibitor)MRP1 (Inhibitor)MRP2 (Inhibitor)MRP3 (Inhibitor)MRP4 (Inhibitor)OATP1A2 (Inhibitor)OATP1B1 (Inhibitor)OATP1B1 (Inhibitor)OATP1B3 (Inhibitor)OATP1B3 (Inhibitor)OATP2B1 (Inhibitor)OCT1 (Inhibitor)OCT2 (Inhibitor)OCTN2 (Inhibitor)P-gp (Inhibitor)MDR1 (Substrate)P-gp (Substrate)

Drug–drug interactions (100+, DDInter)

Interacting drug	Severity	Management
Agalsidase beta	major
Alfuzosin	major
Alimemazine	major
Amiodarone	major
Amisulpride	major
Amitriptyline	major
Amoxapine	major
Anagrelide	major
Apomorphine	major
Arsenic trioxide	major
Asenapine	major
Astemizole	major
Atomoxetine	major
Auranofin	major
Aurothioglucose	major
Azithromycin	major
Bedaquiline	major
Bepridil	major
Bosutinib	major
Buprenorphine	major
Bupropion	major
Cabozantinib	major
Ceritinib	major
Chlorpromazine	major
Cilostazol	major
Ciprofloxacin	major
Cisapride	major
Citalopram	major
Clarithromycin	major
Clofazimine	major
Clomipramine	major
Clozapine	major
Crizotinib	major
Dasatinib	major
Daunorubicin	major
Daunorubicin (liposomal)	major
Deferiprone	major
Desipramine	major
Deutetrabenazine	major
Dextropropoxyphene	major

Showing 40 of 100+.

Registered Products (1)

Brand	Form / strength	Pack	Agent	Citizen (JOD)
Heroquine Syrup	Syrup (as phosphate) BP 1.0 %	60 ml	PHILADELPHIA PHAEMACEUTICALS.COMP/JORDAN	0.800