Clinical Investigation of the Next-Generation Intraocular Lenses

Minimum 22 years of age

Bilateral cataracts for which posterior chamber IOL implantation has been planned

Preoperative best corrected distance visual acuity (BCDVA) of 20/40 Snellen or worse with a glare source or 20/40 Snellen or worse without a glare source

Potential for postoperative BCDVA of 20/30 Snellen or better

Corneal astigmatism:

• Normal corneal topography
• Preoperative corneal astigmatism of 1.00 D or less in both eyes

Clear intraocular media other than cataract in each eye

Availability, willingness and sufficient cognitive awareness to comply with examination procedures

Signed informed consent and HIPAA authorization or equivalent documentation necessary to comply with applicable privacy laws pertaining to medical treatment in the governing countries

Ability to understand and respond to a questionnaire in English

Requiring an intraocular lens power outside the available range of +14.0 D to +26.0 D

Any clinically-significant pupil abnormalities (non-reactive, fixed pupils, or abnormally-shaped pupils)

Irregular corneal astigmatism

Inability to focus or fixate for prolonged periods of time (e.g., due to strabismus, nystagmus, etc.)

Prior corneal refractive (LASIK, LASEK, RK, PRK, etc.) or intraocular surgery. Note: Prophylactic peripheral iridotomies and peripheral laser retinal repairs that, in the opinion of the investigator will not confound study outcome or increase risk to the subject, are acceptable.

Corneal abnormalities such as stromal, epithelial or endothelial dystrophies that are predicted to cause visual acuity losses to a level worse than 20/30 Snellen during the study

Inability to achieve keratometric stability for contact lens wearers (per procedure outlined in Section 10.3)

Recent ocular trauma or ocular surgery that is not resolved/stable or may affect visual outcomes or increase risk to the subject

Subjects with diagnosed degenerative visual disorders (e.g., macular degeneration or other retinal disorders) that are predicted to cause visual acuity losses to a level worse than 20/30 Snellen during the study

Subjects with conditions associated with increased risk of zonular rupture, including capsular or zonular abnormalities that may lead to IOL decentration or tilt, such as pseudoexfoliation, trauma, or posterior capsule defects

Use of systemic or ocular medications that may affect vision

Prior, current, or anticipated use during the course of the 6-month study of tamsulosin or silodosin (e.g., Flomax, Flomaxtra, Rapaflo) that may, in the opinion of the investigator, confound the outcome or increase the risk to the subject (e.g., poor dilation or a lack of adequate iris structure to perform standard cataract surgery)

Poorly-controlled diabetes

Acute, chronic, or uncontrolled systemic or ocular disease or illness that, in the opinion of the investigator, would increase the operative risk or confound the outcome(s) of the study (e.g., immunocompromised, connective tissue disease, suspected glaucoma, glaucomatous changes in the fundus or visual field, ocular inflammation, etc.). Note: controlled ocular hypertension without glaucomatous changes (optic nerve cupping and visual field loss) is acceptable.

Known ocular disease or pathology that, in the opinion of the investigator,

• may affect visual acuity
• may require surgical intervention during the course of the study (macular degeneration, cystoid macular edema, diabetic retinopathy, uncontrolled glaucoma, etc.)
• may be expected to require retinal laser treatment or other surgical intervention during the course of the study (macular degeneration, cystoid macular edema, diabetic retinopathy, etc.)

Patient is pregnant, plans to become pregnant, is lactating or has another condition associated with the fluctuation of hormones that could lead to refractive changes

Concurrent participation or participation within 60 days prior to preoperative visit in any other clinical trial

Desire for monovision correction