Latanoprost

+ 2 more variants

Less Common Side Effects (1 in 100 to 1 in 10)

• Punctate Keratitis: Small areas of inflammation on the surface of the cornea, which may cause sensitivity to light or discomfort.
• Eyelid Redness (Erythema): The skin of the eyelids may become red or inflamed.
• Dry Eye Syndrome: Some patients report a decrease in tear production or a change in the quality of their tears.
• Eye Pain: Mild aching in or around the eye.
• Headache: Systemic absorption can occasionally trigger mild tension-type headaches.

• Iris Hyperpigmentation: This is a unique and significant side effect. Latanoprost can increase the amount of brown pigment in the iris. This change is typically permanent. It is most common in patients with mixed-colored eyes (e.g., blue-brown, grey-brown, or yellow-brown). It is less common in patients with pure blue or pure brown eyes.
• Skin Hyperpigmentation: The skin around the eyes or on the eyelids may darken. This is usually reversible upon discontinuation.
• Asthma Exacerbation: Although rare due to low systemic absorption, some patients with pre-existing asthma have reported worsening of symptoms or shortness of breath (dyspnea).
• Chest Pain (Angina): Very rare reports of chest discomfort have been noted in post-marketing surveillance.

While Latanoprost is a topical medication, certain serious ocular conditions can arise that require urgent evaluation.

> Warning: Stop taking Latanoprost and call your doctor immediately if you experience any of these.

• Macular Edema: Swelling in the central part of the retina (the macula). Symptoms include distorted or blurred central vision. This is more common in patients who have had cataract surgery or who have a torn posterior lens capsule.
• Uveitis or Iritis: Internal eye inflammation. Symptoms include severe eye pain, extreme sensitivity to light (photophobia), and intense redness.
• Severe Allergic Reaction: Symptoms include rash, itching, swelling of the face/tongue/throat, severe dizziness, or trouble breathing.
• Herpetic Keratitis: Reactivation of the herpes simplex virus in the eye. Symptoms include eye pain, redness, and a feeling of a scratch on the cornea.

• Prostaglandin-Associated Periorbitopathy (PAPP): With long-term use, some patients experience a loss of fat around the eye socket. This can lead to a 'sunken eye' appearance (enophthalmos), deepening of the eyelid sulcus, and drooping of the eyelids (ptosis). While some of these changes may reverse after stopping the drug, they can sometimes be persistent.
• Permanent Iris Color Change: As mentioned, the browning of the iris does not go away even if the medication is stopped. This is not considered a 'disease' but is a permanent cosmetic change that patients must be aware of before starting therapy.

No FDA black box warnings for Latanoprost. However, the manufacturer includes strong precautions regarding iris pigmentation and macular edema in the professional labeling.

Report any unusual symptoms, especially changes in your vision or the appearance of your eyes, to your healthcare provider immediately.

Patients using Latanoprost require regular follow-up appointments with their eye care provider. Monitoring typically includes:

• Intraocular Pressure (IOP) Checks: To ensure the medication is effectively lowering the pressure to the target range.
• Optic Nerve Evaluation: Dilated eye exams to check for signs of glaucoma progression.
• Visual Field Testing: To monitor for any loss of peripheral vision.
• Slit-Lamp Examination: To check for signs of inflammation, corneal changes, or iris pigmentation changes.

Latanoprost may cause temporary blurred vision immediately after the drops are instilled. Patients should not drive, operate heavy machinery, or engage in hazardous activities until their vision has cleared. This usually takes only a few minutes.

There are no known direct interactions between Latanoprost and alcohol. However, excessive alcohol consumption can sometimes affect intraocular pressure or general eye health. It is generally safe to consume alcohol in moderation while using Latanoprost eye drops.

Do not stop using Latanoprost without consulting your doctor. Glaucoma is often a 'silent' disease with no symptoms until vision loss occurs. If you stop the medication, your intraocular pressure will likely return to its previous high levels, putting you at risk for permanent optic nerve damage and blindness. There is no 'withdrawal syndrome' associated with Latanoprost, but the rebound in eye pressure is a serious clinical concern.

> Important: Discuss all your medical conditions, especially any history of eye inflammation or herpes infections, with your healthcare provider before starting Latanoprost.

• Topical Beta-Blockers (e.g., Timolol): These are frequently used in combination with Latanoprost. The interaction is beneficial (synergistic), as they lower pressure through different mechanisms. However, patients should be monitored for increased redness or irritation.
• Carbonic Anhydrase Inhibitors (e.g., Dorzolamide): These also have a synergistic effect with Latanoprost. No major negative interaction exists, but ocular comfort should be assessed.

Since Latanoprost is administered topically and systemic absorption is minimal, there are no known interactions with specific foods, including grapefruit, dairy, or high-fat meals. Caffeine consumption can transiently increase intraocular pressure, so patients with glaucoma are often advised to limit excessive caffeine intake, but this is not a direct interaction with the medication itself.

• St. John's Wort: While St. John's Wort affects many systemic drugs via CYP450 enzymes, it is unlikely to have a significant interaction with Latanoprost due to the low systemic levels of the eye drop.
• Omega-3 Fatty Acids: Some evidence suggests Omega-3s may support eye health, but they do not interfere with Latanoprost's mechanism.
• Bilberry/Ginkgo Biloba: These are sometimes taken for eye health. There is no evidence they interact with Latanoprost, but patients should always inform their doctor of all supplements.

Latanoprost is not known to interfere with standard blood or urine laboratory tests. Because it does not reach significant systemic concentrations, it does not affect liver function tests, kidney function tests, or blood counts.

Mechanism of Interactions: Most interactions with Latanoprost are pharmacodynamic (how the drugs affect the eye) rather than pharmacokinetic (how the body processes the drug). For example, the interaction with other prostaglandins is a receptor-level interference where the pressure-lowering effect is blunted by over-saturation of the FP receptors.

> Important: Tell your doctor about ALL medications, supplements, and herbal products you are taking, including other eye drops or ointments.

Patients who have had a severe allergic reaction to other prostaglandin analogs—such as Bimatoprost (Lumigan), Travoprost (Travatan Z), or Tafluprost (Zioptan)—may also be sensitive to Latanoprost. While they are chemically distinct, they belong to the same pharmacological class, and cross-reactivity is possible.

> Important: Your healthcare provider will evaluate your complete medical history, including any previous eye surgeries or infections, before prescribing Latanoprost.

• Clinical Recommendation: Caution should be exercised when Latanoprost is administered to a nursing woman. To minimize potential exposure to the infant, the mother should perform nasolacrimal occlusion for 2 minutes after applying the drops to reduce systemic absorption.

Latanoprost is not FDA-approved for use in pediatric patients. The primary concern in children is the potential for permanent iris color change, which may be more distressing or noticeable in a developing child. Some clinical trials have looked at Latanoprost for pediatric glaucoma, showing it may be less effective in children with primary congenital glaucoma compared to adults with open-angle glaucoma.

No overall differences in safety or effectiveness have been observed between elderly (65 years and older) and younger patients. However, elderly patients may have more difficulty with the manual dexterity required to administer eye drops. They are also more likely to be on multiple medications (polypharmacy), making the 5-minute rule between different eye drops even more important.

Latanoprost has not been specifically studied in patients with renal impairment. However, given that the systemic concentration of the drug is nearly undetectable following ocular administration, no dosage adjustments are necessary for patients with kidney disease or those on dialysis.

Latanoprost has not been studied in patients with hepatic impairment. While the liver is responsible for the metabolism of any drug that reaches the blood, the total amount of Latanoprost in a single drop is so small (1.5 micrograms) that even severely impaired liver function is unlikely to result in toxic systemic levels.

> Important: Special populations require individualized medical assessment. Pregnant or breastfeeding women should always consult their obstetrician and ophthalmologist before using any medicated eye drops.

| Parameter | Value |

|---|---|

| Bioavailability | High ocular penetration (as prodrug) |

| Protein Binding | 87% (Latanoprost acid in plasma) |

| Half-life | 17 minutes (Plasma half-life of active acid) |

| Tmax | 2 hours (in aqueous humor) |

| Metabolism | Hydrolysis in cornea; Beta-oxidation in liver |

| Excretion | Renal >88%, Fecal <5% |

• Molecular Formula: C26H40O5
• Molecular Weight: 432.59 g/mol
• Solubility: Very soluble in acetonitrile; freely soluble in acetone, ethanol, and methanol; practically insoluble in water.
• Structure: Latanoprost is a colorless to slightly yellow oil. It is a prostaglandin F2α analog with a phenyl-substituted aromatic ring at the end of the omega chain, which increases its selectivity for the FP receptor and reduces side effects compared to natural PGF2α.

Latanoprost is classified as a Prostaglandin Analog. Related medications in this class include Bimatoprost (Lumigan), Travoprost (Travatan Z), and Tafluprost (Zioptan). These drugs have largely replaced older classes like beta-blockers (Timolol) and alpha-agonists (Brimonidine) as the first-line therapy for glaucoma due to their superior efficacy and once-daily dosing.