Dorzolamide (Ophthalmic): Complete Drug Monograph

Pharmacokinetic Profile

RBC Washout Half-Life

~4 months (~120 days)

Metabolism

N-de-ethylation to N-desethyl metabolite; stored in RBCs

Protein Binding

~33% (plasma)

Systemic Bioavailability

Very low; plasma generally <15 nM (below assay limit)

Peak Aqueous Humor

~2 hours; ~1000 ng/mL

Clinical Information

Drug Class

Carbonic anhydrase II inhibitor (sulfonamide)

Available Formulations

2% (20 mg/mL) ophthalmic solution

Route

Ophthalmic (topical)

Renal Adjustment

Not recommended if CrCl <30 mL/min

Hepatic Adjustment

Not studied; use with caution

Pregnancy

Use only if benefit justifies risk

Lactation

Present in rat milk; caution advised

Schedule

Prescription only (not controlled)

Generic Available

Yes

Sulfonamide

Yes — cross-reactivity risk with sulfa allergy

Indications

Indication	Approved Population	Therapy Type	Status
Open-angle glaucoma — elevated IOP	Adults and paediatric patients	Monotherapy or adjunctive	FDA Approved
Ocular hypertension — IOP reduction	Adults and paediatric patients	Monotherapy or adjunctive	FDA Approved

Dorzolamide was the first topical carbonic anhydrase inhibitor (CAI) approved for ophthalmic use (FDA approval 1994). It was developed through structure-based drug design to deliver the IOP-lowering benefits of systemic CAIs (such as acetazolamide) via a topical route, thereby avoiding the significant systemic adverse effects associated with oral agents. In clinical studies, dorzolamide lowered IOP by approximately 3–5 mmHg throughout the day, and this effect was consistent for up to one year. Dorzolamide is primarily used as adjunctive therapy when prostaglandin analogues or beta-blockers alone do not achieve target IOP, and it is available in a fixed-dose combination with timolol (Cosopt) for improved adherence.

Off-Label Uses

Cystoid macular oedema (CME): Topical dorzolamide has been used off-label for the management of macular oedema associated with conditions such as retinitis pigmentosa and post-surgical CME, based on its ability to inhibit carbonic anhydrase in the retinal pigment epithelium and enhance fluid absorption. (Evidence quality: Low)

Paediatric glaucoma: Although not carrying a formal paediatric age restriction, dorzolamide is used in paediatric patients including infants, supported by a 3-month controlled trial demonstrating a comparable adverse reaction profile to adults. (Evidence quality: Moderate)

Dose

Dorzolamide Dosing

Clinical Scenario	Starting Dose	Maintenance Dose	Maximum Dose	Notes
Open-angle glaucoma or ocular hypertension — monotherapy	1 drop 2% in affected eye(s) TID	Same as starting dose	1 drop TID	Expected IOP reduction: 3–5 mmHg Efficacy of less-than-TID dosing not established (FDA PI)
Adjunctive therapy — with prostaglandin analogue, beta-blocker, or alpha-agonist	1 drop 2% in affected eye(s) TID	Same as starting dose	1 drop TID	Separate all topical drops by at least 5 minutes Provides additive IOP lowering when combined with other classes
Fixed combination with timolol (Cosopt) — adults	1 drop (dorzolamide 2%/timolol 0.5%) in affected eye(s) BID	Same as starting dose	1 drop BID	Simplifies regimen from dorzolamide TID + timolol BID See Cosopt PI for complete prescribing details
Paediatric glaucoma	1 drop 2% in affected eye(s) TID	Same as starting dose	1 drop TID	Safety demonstrated in 3-month controlled paediatric trial Adverse reaction profile comparable to adults (FDA PI)

Clinical Pearl: Bitter Taste After Instillation

Approximately 25% of patients experience a bitter or unusual taste following dorzolamide instillation, caused by the drug draining through the nasolacrimal duct into the oropharynx. Applying nasolacrimal occlusion (digital pressure at the inner canthus for 1–2 minutes) after each drop significantly reduces this side effect as well as systemic absorption. This is a common reason for patient dissatisfaction and should be proactively addressed during counselling.

Administration Guidance

Remove contact lenses before instillation and wait at least 15 minutes before reinserting — the solution contains benzalkonium chloride 0.0075%, which can be absorbed by and discolour soft contact lenses. When using multiple topical ophthalmic products, separate each by at least 5 minutes. Store at 15–30°C. Protect from light. After opening, use until the expiration date on the bottle.

Pharmacology

Mechanism of Action

Dorzolamide hydrochloride is a potent inhibitor of human carbonic anhydrase II (CA-II), with approximately 4,000-fold selectivity over CA-I. Carbonic anhydrase is an enzyme found in many body tissues including the ciliary processes of the eye, where it catalyses the reversible hydration of carbon dioxide to bicarbonate. In the ciliary epithelium, inhibition of CA-II reduces bicarbonate ion formation, which decreases sodium and fluid transport into the posterior chamber, ultimately reducing aqueous humour secretion and lowering IOP. Unlike systemic CAIs such as acetazolamide, topical dorzolamide achieves therapeutic concentrations in the ciliary processes (2–10 μM) while maintaining plasma free drug concentrations approximately 200-fold lower than those needed for systemic effects, providing a favourable local-to-systemic activity ratio.

ADME Profile

Parameter	Value	Clinical Implication
Absorption	Corneal absorption; peak aqueous humour concentration ~1000 ng/mL at ~2 h after topical 2%; plasma concentrations generally below assay limit (<15 nM)	Excellent local ocular bioavailability with minimal systemic exposure; avoids metabolic acidosis and electrolyte disturbances seen with oral CAIs
Distribution	Accumulates in RBCs by binding to CA-II (reaching 20–25 μM at steady state, ~8 days); plasma protein binding ~33%; plasma concentration ~0.034 μM (1/700 of RBC level)	RBC accumulation is the primary systemic reservoir; steady-state RBC concentrations reflect CA-II saturation rather than toxicity risk
Metabolism	Single N-desethyl metabolite formed; also binds to RBC carbonic anhydrase (primarily CA-I); less potent CA-II inhibitor than parent	Metabolite is pharmacologically less active; both parent and metabolite accumulate in RBCs and are slowly cleared
Elimination	Primarily renal excretion (unchanged drug + metabolite); RBC washout t½ ~4 months (~120 days); at steady state, renal excretion ~1.3 mg/day with renal clearance ~90 mL/min	Very long RBC elimination half-life; however, plasma free drug is too low to cause systemic CAI effects in healthy individuals; avoid in severe renal impairment (CrCl <30 mL/min)

Side Effects

≥10%Very Common

Adverse Effect	Incidence	Clinical Note
Ocular burning, stinging, or discomfort	~33% (1 in 3 patients)	Occurs immediately following instillation; usually transient; most frequent adverse reaction
Bitter taste (dysgeusia)	~25% (1 in 4 patients)	Due to nasolacrimal drainage to oropharynx; reduced by nasolacrimal occlusion; common reason for patient complaint
Superficial punctate keratitis	10–15%	May be partly attributable to BAK preservative or low pH (5.6) of solution; monitor corneal surface
Ocular allergic reaction (signs and symptoms)	~10%	May present as conjunctivitis, lid reactions, or contact allergy; may resolve on discontinuation

1–5%Common

Adverse Effect	Incidence	Clinical Note
Conjunctivitis / lid reactions	1–5%	Chronic use may cause allergic-type reactions; resolve on discontinuation; evaluate before restarting (FDA PI)
Blurred vision	1–5%	Transient; may occur with instillation
Eye redness	1–5%	Mild conjunctival hyperemia
Tearing	1–5%	Reflex lacrimation; self-resolving
Dryness / photophobia	1–5%	May need sunglasses for photophobia; artificial tears for dryness

SeriousSerious (Regardless of Frequency)

Adverse Effect	Estimated Frequency	Typical Onset	Required Action
Stevens-Johnson syndrome / toxic epidermal necrolysis	Very rare (sulfonamide class effect)	Days to weeks after initiation	Immediate discontinuation; emergency dermatology/medical care; fatalities reported (FDA PI). Sensitisation may recur on re-exposure regardless of route
Blood dyscrasias (agranulocytosis, aplastic anaemia)	Very rare (sulfonamide class effect)	Variable	Discontinue immediately; haematology referral; monitor blood counts
Fulminant hepatic necrosis	Very rare (sulfonamide class effect)	Variable	Discontinue; hepatology assessment; fatalities reported
Corneal oedema / decompensation	Uncommon; higher risk with low endothelial cell counts	Weeks to months	Monitor corneal thickness; discontinue if corneal oedema develops; avoid in patients with compromised corneal endothelium
Choroidal detachment (post-filtration surgery)	Rare (postmarketing)	Post-surgical	Ophthalmology assessment; may require discontinuation of aqueous suppressant therapy
Urolithiasis	Rare	Variable	Assess for renal calculi; CAI class effect from altered urinary pH and citrate excretion; consider discontinuation

DiscontinuationTreatment Discontinuation

Overall Tolerability

Moderate

Top reasons: Ocular burning/stinging, bitter taste, and allergic conjunctivitis/lid reactions

Clinical Context

Comparable to adults in children

The 3-month paediatric trial showed an adverse reaction profile comparable to adults, supporting continued paediatric use

Reason for Discontinuation	Incidence	Context
Ocular burning/stinging/discomfort	Leading ocular reason	Occurs in ~1/3 of patients; most tolerate with continued use but a subset discontinue
Bitter taste	Common patient complaint	Affects ~1/4 of patients; reducible with nasolacrimal occlusion technique
Allergic conjunctivitis / lid reactions	Reported with chronic use	FDA PI recommends discontinuation and evaluation before considering rechallenge

Sulfonamide Cross-Reactivity Warning

Dorzolamide contains a sulfonamide moiety and is absorbed systemically despite topical administration. The FDA PI warns that the same types of severe reactions attributable to systemic sulfonamides may occur, including Stevens-Johnson syndrome, toxic epidermal necrolysis, fulminant hepatic necrosis, agranulocytosis, aplastic anaemia, and other blood dyscrasias. Fatalities have been reported, although rarely. Sensitisation may recur when a sulfonamide is re-administered regardless of route. Before prescribing, ask about sulfonamide allergy. If signs of serious reactions or hypersensitivity occur, discontinue immediately.

Int

Drug Interactions

Dorzolamide has a limited systemic drug interaction profile due to very low plasma concentrations. The principal concerns relate to additive carbonic anhydrase inhibition when combined with oral CAIs and potential acid-base disturbances with high-dose salicylates.

MajorOral Carbonic Anhydrase Inhibitors (acetazolamide, methazolamide)

MechanismAdditive systemic CA inhibition from combined topical and oral routes

EffectIncreased risk of systemic CAI effects including metabolic acidosis, electrolyte disturbances (hypokalaemia), and renal effects

ManagementConcomitant use is NOT recommended (FDA PI). If both are deemed essential, monitor serum electrolytes and bicarbonate closely

FDA PI §7.1

ModerateHigh-Dose Salicylates (aspirin ≥3 g/day)

MechanismOral CAIs cause acid-base disturbances that can alter salicylate distribution; salicylate toxicity may increase

EffectPotential for increased salicylate toxicity (CNS effects, metabolic acidosis)

ManagementAlthough not reported in clinical trials with topical dorzolamide, the theoretical risk exists; monitor if high-dose salicylates are co-prescribed

FDA PI §7.2

MinorOther Topical Ophthalmic Drugs

MechanismDilution or washout effect if administered too close together

EffectReduced efficacy of either agent if not adequately separated

ManagementAdminister at least 5 minutes apart (FDA PI)

FDA PI §2

Mon

Monitoring

Intraocular PressureBaseline; 2–4 weeks; then every 3–6 months
RoutineExpected IOP reduction: 3–5 mmHg. Effect consistent throughout the day. Efficacy with less-than-TID dosing has not been established.
Corneal EndotheliumBaseline (specular microscopy if risk factors); periodically
Trigger-basedCA activity in corneal endothelium means CAI use carries risk of corneal oedema in patients with low endothelial cell counts. A 1-year study showed ~4% mean endothelial cell loss. Monitor corneal thickness if symptoms arise (hazy vision, haloes).
Ocular Surface / Allergy SignsEach visit
RoutineMonitor for conjunctivitis, lid reactions, and punctate keratitis. Allergic-type reactions reported with chronic use may resolve on discontinuation. Evaluate before considering rechallenge.
Sulfonamide Hypersensitivity SignsAt initiation and each visit
Trigger-basedAsk about skin rash, mucosal lesions, fever, or systemic symptoms. Discontinue immediately if SJS/TEN or other serious sulfonamide reaction suspected.
Renal FunctionBaseline; as clinically indicated
Trigger-basedDrug is not recommended in severe renal impairment (CrCl <30 mL/min) due to predominant renal excretion. Check renal function in elderly or those with comorbidities.
Visual FieldsPer glaucoma guidelines (every 6–12 months)
RoutineStandard automated perimetry for glaucomatous progression. Not specific to dorzolamide but essential for overall glaucoma management.

Contraindications & Cautions

Absolute Contraindications

Hypersensitivity to dorzolamide, any component of the product, or other sulfonamides (FDA PI Section 4)

Relative Contraindications (Specialist Input Recommended)

Severe renal impairment (CrCl <30 mL/min) — drug and metabolite excreted renally; not recommended by FDA PI (Section 8.6)
Low corneal endothelial cell count — increased risk of corneal oedema due to CA inhibition in corneal endothelium; use with caution (FDA PI Section 5.3)
Concurrent oral CAI therapy — additive systemic CA inhibition; concomitant use not recommended (FDA PI Section 7.1)
Pregnancy — fetal vertebral malformations in rabbits at 37x clinical exposure; use only if benefit justifies risk (FDA PI Section 8.1)

Use with Caution

History of sulfonamide allergy — although true cross-reactivity between ophthalmic CAIs and systemic sulfonamides is debated, the FDA PI includes the sulfonamide class warning
Hepatic impairment — not studied; use with caution (FDA PI Section 8.6)
Acute angle-closure glaucoma — additional therapeutic interventions are required beyond IOP-lowering agents (FDA PI Section 5.5)
Contact lens wearers — BAK 0.0075% may discolour soft lenses; remove before instillation, reinsert after 15 minutes
Breastfeeding — dorzolamide detected in milk of lactating rats; not known if excreted in human milk; weigh risk-benefit

FDA Class-Wide Regulatory Warning Sulfonamide-Containing Ophthalmic Products — Serious Hypersensitivity Reactions

Dorzolamide is a sulfonamide, and although administered topically, it is absorbed systemically. The FDA PI carries a warning that the same types of adverse reactions attributable to sulfonamides may occur with topical administration, including fatalities from Stevens-Johnson syndrome, toxic epidermal necrolysis, fulminant hepatic necrosis, agranulocytosis, aplastic anaemia, and other blood dyscrasias. Sensitisation may recur when a sulfonamide is re-administered irrespective of the route. If signs of serious reactions or hypersensitivity occur, dorzolamide must be discontinued immediately.

Patient Counselling

Purpose of Therapy

Dorzolamide eye drops are prescribed to lower the pressure inside the eye and protect against vision loss from glaucoma. The drops work by reducing the amount of fluid produced inside the eye. This medication controls the condition but does not cure it, so it must be used consistently three times daily, approximately 8 hours apart.

How to Take

Instil one drop into the affected eye(s) three times daily. After each drop, close the eye and press a fingertip against the inner corner of the eye near the nose for 1–2 minutes to reduce bitter taste and systemic absorption. If using other eye drops, wait at least 5 minutes between each. Remove contact lenses before use and wait 15 minutes before reinserting.

Bitter Taste

Tell patientAbout 1 in 4 patients notice a bitter or unusual taste after putting in the drops. This happens because the medication can drain through the tear duct into the back of the throat. Pressing gently on the inner corner of the eye for 1–2 minutes after instillation helps prevent this.

Call prescriberIf the taste is persistently bothersome and nasolacrimal occlusion does not help, discuss with your doctor as alternative medications are available.

Stinging and Burning

Tell patientBrief stinging or burning when putting in the drop is common (about 1 in 3 patients) and normally settles within a minute. This is the most frequently reported side effect and usually becomes less noticeable with continued use.

Call prescriberIf burning is severe, persistent, or accompanied by increasing redness, swelling of the eyelids, or itching, stop the drops and contact your eye doctor as this may indicate an allergic reaction.

Sulfa Allergy

Tell patientThis medication belongs to the sulfonamide family. If you have ever had a serious allergic reaction to a sulfa antibiotic or other sulfa-containing medication, inform your doctor before starting these drops. While serious reactions are very rare with the eye drops, they have been reported.

Call prescriberSeek immediate medical attention if you develop a skin rash, blistering, fever, sore throat, mouth sores, or any signs of a severe allergic reaction after starting this medication.

Vision Changes

Tell patientBrief blurred vision may occur after instilling the drops. Avoid driving or operating machinery until vision clears. Increased sensitivity to light has also been reported; sunglasses may help.

Call prescriberIf you notice persistent hazy or foggy vision, haloes around lights, or worsening visual acuity, contact your eye doctor as these may indicate corneal changes that require assessment.

Ref

Sources

Regulatory (PI / SmPC)

Trusopt (dorzolamide hydrochloride ophthalmic solution) 2% — Full Prescribing Information (Merck). NDA 20408/S-052, revised December 2020. accessdata.fda.govPrimary source for all FDA-approved indications, dosing, contraindications, adverse reactions, PK data, and drug interactions used in this monograph.
Dorzolamide hydrochloride ophthalmic solution 2% — Full Prescribing Information (generic, Sagent). Revised January 2026. drugs.comGeneric dorzolamide PI with identical clinical data; confirms adverse reaction rates and administration guidance.

Key Clinical Trials

Strahlman E, Tipping R, Vogel R; International Dorzolamide Study Group. A double-masked, randomized 1-year study comparing dorzolamide, timolol, and betaxolol. Arch Ophthalmol. 1995;113(8):1009–1016. PMID: 7639651.Major 1-year comparative trial establishing dorzolamide TID as an effective IOP-lowering agent with acceptable tolerability vs beta-blockers.
Wilkerson M, Cyrlin M, Lippa EA, et al. Four-week safety and efficacy study of dorzolamide, a novel, active topical carbonic anhydrase inhibitor. Arch Ophthalmol. 1993;111(10):1343–1350. PMID: 8216014.Early phase clinical trial establishing safety and dose-response characteristics of topical dorzolamide.
Lippa EA, Carlson LE, Ehinger B, et al. Dose response and duration of action of dorzolamide, a topical carbonic anhydrase inhibitor. Arch Ophthalmol. 1992;110(4):495–499. PMID: 1562255.Dose-finding study establishing the 2% concentration as optimal for the balance of IOP efficacy and tolerability.

Guidelines

European Glaucoma Society. Terminology and Guidelines for Glaucoma. 5th Edition. 2020. eugs.orgCurrent EGS guidelines positioning topical CAIs as adjunctive agents in glaucoma management.
American Academy of Ophthalmology. Preferred Practice Pattern: Primary Open-Angle Glaucoma. 2020. aao.orgUS guideline discussing dorzolamide as second-line adjunctive therapy.

Mechanistic / Basic Science

Sugrue MF. Pharmacological and ocular hypotensive properties of topical carbonic anhydrase inhibitors. Prog Retin Eye Res. 2000;19(1):87–112. PMID: 10614681.Comprehensive review of topical CAI pharmacology including dorzolamide’s selectivity for CA-II and mechanism of aqueous suppression.
Maren TH, Conroy CW. A new class of carbonic anhydrase inhibitor. J Biol Chem. 1993;268(35):26233–26239. PMID: 8253744.Foundational biochemistry establishing dorzolamide’s high-affinity binding to CA-II and the structure-activity relationships underlying topical CAI design.

Pharmacokinetics / Special Populations

Maren TH, Bar-Ilan A, Conroy CW, Brechue WF. Chemical and pharmacological properties of MK-927, a sulfonamide carbonic anhydrase inhibitor that accumulates in the eye. Exp Eye Res. 1990;50(1):27–36. PMID: 2307710.Preclinical PK study of dorzolamide demonstrating corneal penetration, ciliary body concentrations, and the red blood cell accumulation kinetics.
Biollaz J, Munafo A, Buclin T, et al. Whole-blood pharmacokinetics and metabolic effects of the topical carbonic anhydrase inhibitor dorzolamide. Eur J Clin Pharmacol. 1995;47(5):453–460. PMID: 7720769.RCT in healthy volunteers quantifying RBC washout half-life of ~120 days and confirming absence of clinically significant metabolic or renal effects with topical dosing.
Maren TH, Brechue WF, Bar-Ilan A. Relations among IOP reduction, ocular disposition and pharmacology of the carbonic anhydrase inhibitor ethoxzolamide. Exp Eye Res. 1992;55(1):73–79. PMID: 1397132.Comparative PK data providing context for dorzolamide’s local-to-systemic concentration ratio advantage over oral CAIs.
Schmitz K, Banditt P, Motschmann M, Meyer FP, Behrens-Baumann W. Population pharmacokinetics of 2% topical dorzolamide in the aqueous humor of humans. Invest Ophthalmol Vis Sci. 1999;40(7):1621–1624. PMID: 10359348.Human aqueous humor PK study confirming peak dorzolamide concentrations of ~1000 ng/mL at approximately 2 hours after topical application.
Pfeiffer N. Dorzolamide: development and clinical application of a topical carbonic anhydrase inhibitor. Surv Ophthalmol. 1997;42(2):137–151. PMID: 9381368.Comprehensive clinical review of dorzolamide covering development history, PK, efficacy data, and its role in the glaucoma treatment ladder.