Autosomal Dominant Vitreoretinochoroidopathy (ADVIRC) with Nanophthalmos

Dr. Reem Saadeh Haddad, MD - Clinical Genetics, Genomics, Cytogenetics, Biochemical Genetics Specialist Dr. Reem Saadeh Haddad, MD - Clinical Genetics, Genomics, Cytogenetics, Biochemical Genetics Specialist
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Rx Eye & Vision Care (A - Z)

Autosomal dominant vitreoretinochoroidopathy (ADVIRC) with nanophthalmos is a rare, inherited eye disorder. “Autosomal dominant” means a single changed gene from one parent can cause the condition in a child. “Vitreoretinochoroidopathy” describes problems in three parts of the eye: the gel (vitreous), the light-sensing layer (retina), and the blood-rich layer behind it (choroid). “Nanophthalmos” means the eyeball is smaller than usual in all dimensions, often leading to strong farsightedness. People with ADVIRC typically develop a dark, circular band of pigment in the far edge of the retina, along with fine white dots and thread-like changes in the vitreous. The disease tends to progress slowly over many years. Some people have additional developmental eye changes such as microcornea, shallow front chamber, angle-closure glaucoma, cataracts, and optic nerve changes. Many cases are caused by changes (variants) in a gene called BEST1 (historically VMD2), which is active in the retinal pigment epithelium (RPE), a supportive cell layer vital for retinal health. In some families with ADVIRC, nanophthalmos is also present, linking the retinal disease to the small-eye growth pattern and high hyperopia. MedlinePlus+3PMC+3Orpha+3

Most people with ADVIRC have a change (variant) in the BEST1 gene. This gene makes the bestrophin-1 protein in the RPE, which helps control chloride ion movement. Different BEST1 variants can cause several “bestrophinopathies,” including Best disease, adult-onset vitelliform dystrophy, ADVIRC, and autosomal-recessive bestrophinopathy. In ADVIRC, BEST1 variants disrupt RPE function and lead to the typical peripheral pigment band and other retinal changes. NCBI+1

Some people with ADVIRC also have nanophthalmos—a very small eye with a short axial length and high far-sightedness (hyperopia). The eye has a thicker sclera and a shallow front chamber, which raises the risk of angle-closure glaucoma and uveal effusion (fluid under the choroid). These structural issues make cataract or glaucoma surgery more risky and need special planning. EyeWiki+1

Other names

Doctors and articles may use different names that refer to the same or closely related conditions:

  • ADVIRC (short form of autosomal dominant vitreoretinochoroidopathy). Orpha

  • BEST1-associated retinopathy or bestrophinopathy spectrum, because the BEST1 gene is involved in several related disorders. NCBI

  • Peripheral annular pigmentary dystrophy, highlighting the hallmark ring-shaped pigment band in the retinal periphery. ScienceDirect

  • VMD2-related disease, using the older gene name for BEST1. IOVS

Types

Because this disease is rare and variable, doctors often group patients by clinical patterns rather than strict subtypes. These patterns help plan monitoring and care:

  1. Classic ADVIRC pattern. The peripheral, circular hyperpigmented band with a sharp border is present, visual function declines slowly, and the central retina may be relatively preserved for many years. PMC+1

  2. ADVIRC with developmental eye changes. In addition to the pigment band, there may be microcornea, presenile cataract, shallow anterior chamber, iris dysgenesis, angle-closure glaucoma, or optic nerve dysplasia. Visual problems can appear earlier due to these added features. PMC+1

  3. ADVIRC with nanophthalmos (the focus here). The eye is small in all dimensions, causing high hyperopia and a tendency to narrow angles and angle-closure glaucoma. The small eye coexists with the retinal pigment ring and vitreous changes typical of ADVIRC. PubMed+1

  4. BEST1-spectrum overlap. Some families show features that overlap with other bestrophinopathies (e.g., Best vitelliform macular dystrophy or adult-onset vitelliform). Genetic testing clarifies the diagnosis. NCBI

Causes

Although this is one genetic condition, it helps to break “cause” into gene changes, cellular effects, eye-development effects, and disease modifiers—all of which “cause” the final picture you see clinically.

  1. BEST1 pathogenic variants. ADVIRC usually results from changes in the BEST1 gene, which encodes the protein bestrophin-1 in RPE cells. MedlinePlus+1

  2. Aberrant pre-mRNA splicing. Several ADVIRC variants disrupt normal splicing of BEST1, altering the protein sequence or amount. IOVS+1

  3. Abnormal chloride/calcium-activated channel function. Bestrophin-1 likely acts as or regulates an ion channel in the RPE; altered channel behavior affects fluid and metabolite handling for photoreceptors. (Inference from BEST1 biology summarized in reviews.) NCBI

  4. RPE dysfunction. When RPE cells do not transport fluid or support photoreceptors normally, retinal degeneration and pigment changes occur over time. NCBI

  5. Vitreous interface changes. ADVIRC includes fibrillar condensations in the vitreous, likely a downstream effect of retinal/RPE changes. Orpha

  6. Peripheral retinal remodeling. The annular hyperpigmented band reflects chronic remodeling of the outer retina and RPE at the periphery. PMC

  7. Ocular developmental pathway effects. Some BEST1 variants correlate with developmental anomalies (microcornea, iris changes), suggesting BEST1 has roles beyond the adult RPE. PMC

  8. Nanophthalmos gene overlap. Nanophthalmos is linked to several genes (MFRP, PRSS56, TMEM98, CRB1, BEST1). In some ADVIRC families, BEST1 variants travel with the small-eye phenotype. PMC+1

  9. High hyperopia from short axial length. A shorter eye focuses images behind the retina, causing high farsightedness and setting up narrow angles. EyeWiki

  10. Angle crowding leading to glaucoma. Small eyes and shallow chambers predispose to angle-closure glaucoma, which can further reduce vision. PMC

  11. Cataract formation. Presenile cataracts occur more often in ADVIRC families, adding to blur and glare. PMC

  12. Iris/anterior segment anomalies. Iris dysgenesis and related changes can accompany the small eye and narrow angles. Nature

  13. Optic nerve development differences. Some cases show optic nerve dysplasia, which may limit vision even if the retina is relatively stable. Nature

  14. Dominant inheritance. A single altered BEST1 copy is enough to cause disease; each child has ~50% risk if a parent is affected. (Standard autosomal dominant genetics summarized in sources.) NCBI

  15. Allelic heterogeneity. Different BEST1 variants can produce varied severity or combinations of features. Nature

  16. Intra-familial variability. Even with the same variant, severity can differ widely among relatives, implying other modifiers. PMC

  17. Potential dominant-negative or dosage effects. Some variants may interfere with normal protein or reduce effective protein, changing RPE function (mechanistic models discussed in reviews). NCBI

  18. Secondary photoreceptor stress. When RPE support is impaired, rods and cones suffer, eventually affecting night and day vision. NCBI

  19. Vascular/RPE barrier alterations. Subtle changes in the RPE and choroid can alter the outer blood-retina barrier, contributing to pigment and autofluorescence patterns. (General bestrophinopathy mechanisms.) NCBI

  20. Life-long cumulative change. Because the condition is slowly progressive, small early effects compound over decades, explaining late visual field narrowing even when central vision stays good for years. PMC

Symptoms

  1. Blurry distance vision from childhood or teens due to strong farsightedness in nanophthalmos; glasses often help but not fully. EyeWiki

  2. Eye strain and headaches from the effort to focus through high hyperopia; near work can be tiring. EyeWiki

  3. Glare and halos, especially if a cataract develops early. PMC

  4. Intermittent eye pain or brow ache, sometimes with transient blur, can signal angle crowding or angle-closure attacks. This is urgent. PMC

  5. Reduced night vision or trouble in dim light as peripheral retina gradually loses function. PMC

  6. Gradual loss of side vision, reflecting constriction of visual fields over time. PMC

  7. Sensitivity to bright light and slow adaptation when moving from bright to dim rooms. (RPE/photoreceptor stress is common in bestrophinopathies.) NCBI

  8. Floaters or thread-like shapes, consistent with vitreous fibrillar condensations. Orpha

  9. Color vision changes later in the disease in some people, as cone function is affected. (General bestrophinopathy behavior.) NCBI

  10. Reduced contrast sensitivity, making low-contrast scenes (fog, dusk) harder to see. (RPE/outer retina involvement.) NCBI

  11. Visual fluctuations, worse with fatigue or glare, better with fresh lighting and rest. (Common in retinal dystrophies.)

  12. Early need for strong glasses or contact lenses due to high hyperopia; some choose refractive solutions only if safe for small-eye anatomy. EyeWiki

  13. Amblyopia risk (lazy eye) if high hyperopia or anisometropia is not corrected in childhood. (Standard pediatric optics consideration in small eyes.) EyeWiki

  14. Episodes of redness and nausea with vision dimming may accompany acute angle closure—a medical emergency. EyeWiki

  15. Family history of similar eye issues, often with variable severity in relatives, matching autosomal dominant inheritance. NCBI

Diagnostic tests

A) Physical exam and basic clinical measures

  1. Best-corrected visual acuity. Measures how clearly you see with optimal lenses; tracks central vision over time. Many people retain fair central acuity for years while side vision narrows. PMC

  2. Objective and subjective refraction. Finds the right farsighted correction, often high in nanophthalmos; may reduce headaches and eye strain. EyeWiki

  3. Intraocular pressure (IOP). Important because crowded angles raise the risk of angle-closure glaucoma; pressure checks at each visit help prevent optic nerve damage. PMC

  4. Confrontation visual fields or automated perimetry. Detects peripheral field loss typical of ADVIRC over time; guides counseling and safety planning. PMC

  5. Color vision testing. Can show cone-related changes later in disease; provides a functional baseline. (Bestrophinopathy spectrum.) NCBI

B) Manual/clinical slit-lamp and ophthalmoscopic tests

  1. Slit-lamp biomicroscopy. Examines the cornea, anterior chamber depth, iris, and lens; looks for microcornea, shallow chamber, iris anomalies, and early cataract. PMC

  2. Gonioscopy. Directly inspects the drainage angle; narrow or closed angles are common in small eyes and guide decisions about laser peripheral iridotomy or other steps. PMC

  3. Dilated fundus examination with indirect ophthalmoscopy. Shows the peripheral, annular pigment band and punctate white opacities; tracks any new changes or risks. Orpha

  4. Scleral depression in the periphery (as appropriate). Helps view extreme periphery in small eyes; confirms the full concentric pigment ring and any vitreous adhesions. University College London

  5. Lens grading (cataract). Early detection of presenile cataract supports timely counseling and surgical planning if vision suffers. PMC

C) Laboratory / genetic and pathological tests

  1. Genetic testing of BEST1. Pinpoints the causative variant, confirms diagnosis within the bestrophinopathy spectrum, and supports family counseling (autosomal dominant risk). NCBI+1

  2. Segregation analysis in relatives. Testing relatives clarifies who is at risk and can reveal why severity differs within a family. PMC

  3. Expanded nanophthalmos panel (MFRP, PRSS56, TMEM98, CRB1, others) when phenotype is mixed. Helpful if features suggest a broader small-eye syndrome beyond BEST1. PMC

  4. Research-level RPE functional assays (not routine). Scientific studies show BEST1 variants alter RPE ion transport/splicing, helping explain disease biology. Metrovision

D) Electrodiagnostic tests

  1. Full-field electroretinogram (ERG). Measures overall rod and cone function; ADVIRC often shows reduced retinal responses that track disease extent. PMC

  2. Electro-oculogram (EOG). Assesses RPE function; in bestrophinopathies the Arden ratio may be abnormal, supporting an RPE-based disorder. NCBI

E) Imaging and biometric tests

  1. Optical coherence tomography (OCT) of macula and periphery (wide-field when possible). Maps retinal layers and the RPE; shows thinning or disruptions and can visualize the sharp border between pigmented and more normal retina. University College London

  2. Fundus autofluorescence (FAF). Highlights lipofuscin/RPE signals; the peripheral annular band usually has a characteristic autofluorescence pattern that helps follow progression. PMC

  3. Biometry / axial length measurement (A-scan or optical biometer). Confirms short axial length in nanophthalmos, supports safe surgical planning, and helps choose intraocular lenses if cataract surgery is needed. EyeWiki

  4. Anterior segment imaging (ultrasound biomicroscopy or anterior-segment OCT). Quantifies anterior chamber depth, iris-lens configuration, and angle width to estimate angle-closure risk and to plan laser iridotomy or other procedures if indicated. EyeWiki

Non-pharmacological treatments (therapies & others)

  1. Genetic counseling and family screening
    Description. A trained counselor explains the autosomal-dominant pattern, test options for BEST1, and what results mean for relatives. Counseling covers family planning and helps identify at-risk relatives for eye checks. Purpose. To inform choices, detect disease earlier in relatives, and reduce anxiety. Mechanism. Education plus targeted genetic testing to find BEST1 variants that track with ADVIRC in the family. NCBI

  2. Regular comprehensive eye exams (lifetime)
    Description. Yearly to 6-monthly checks with dilated exam, IOP measurement, and imaging (OCT, autofluorescence, widefield photos) to watch the pigment band, macula, and optic nerve. Purpose. To catch treatable problems (glaucoma, cystoid macular edema, CNV) early. Mechanism. Surveillance and early intervention reduce permanent damage. PubMed+1

  3. Electrophysiology as needed (EOG/ERG)
    Description. If the diagnosis is unclear or to monitor RPE function, an EOG (Arden ratio) and ERG can help. Purpose. To support diagnosis within the bestrophinopathy spectrum and track function. Mechanism. Measures RPE light response and global retinal activity. EyeWiki+1

  4. Angle-closure glaucoma prevention (laser peripheral iridotomy when indicated)
    Description. People with nanophthalmos have shallow chambers and narrow angles. An eye doctor may do a laser hole in the iris to prevent acute angle closure. Purpose. To prevent dangerous eye-pressure spikes. Mechanism. Creates a bypass for fluid from the back to the front of the eye, opening the angle. EyeWiki

  5. Careful surgical planning in nanophthalmos
    Description. If cataract or other intraocular surgery is needed, the team plans scleral windows (sclerostomies) before entering the eye to lower the risk of uveal effusion. Anesthesia, wound design, viscoelastics, and IOL power choices are adapted to small eyes. Purpose. To avoid choroidal effusion and vision-threatening complications. Mechanism. Scleral windows reduce fluid build-up under the choroid during/after surgery. EyeWiki+1

  6. Uveal effusion management (non-drug steps)
    Description. Positioning, observation, stopping traction, and, if surgery is planned, pre-emptive scleral windows; vitrectomy is usually secondary in nanophthalmos. Purpose. To reattach tissues and protect vision. Mechanism. Improves choroidal fluid outflow through sclera; reduces suprachoroidal fluid. EyeWiki

  7. Low-vision rehabilitation
    Description. Training with magnifiers, lighting, high-contrast materials, large-print devices, and digital accessibility. Purpose. To maintain independence and quality of life. Mechanism. Optical and environmental adaptations improve usable vision despite retinal disease. NORD

  8. Blue-light and UV protection
    Description. Sunglasses with UV protection and optional blue-light filtering for outdoor use. Purpose. To protect RPE/retina from cumulative light stress. Mechanism. Filters harmful wavelengths that may worsen retinal stress over decades. NCBI

  9. Treat macular edema with non-drug measures first (monitor, triggers)
    Description. Identify and stop potential triggers (e.g., certain chemo drugs) when medically possible; optimize systemic control (blood pressure, diabetes). Purpose. To avoid or reduce CME before adding medicines. Mechanism. Removing aggravating factors can reduce retinal fluid. BioMed Central+1

  10. Occupational therapy for daily tasks
    Description. Home and workplace modifications, labeling systems, and task lighting. Purpose. To keep daily activities safe and efficient. Mechanism. Environmental and task redesign to match visual ability. NORD

  11. Educational support (for children)
    Description. School accommodations (large print, seating, devices). Purpose. To help children with inherited retinal disease learn well. Mechanism. Accessibility tools reduce the impact of reduced acuity or field. NCBI

  12. Driving and mobility counseling
    Description. Vision standards review, adaptive strategies, and alternative transport planning if needed. Purpose. Safety and legal compliance. Mechanism. Aligns mobility with functional vision and driving laws. NORD

  13. Home fall-prevention for glaucoma risk
    Description. Remove tripping hazards, improve lighting, use high-contrast steps. Purpose. Reduce injury if peripheral vision declines. Mechanism. Environmental changes reduce fall risk linked to field loss. FDA Access Data

  14. Nutritional counseling for eye and general health
    Description. Balanced diet rich in leafy greens, colored fruits/vegetables, and omega-3 sources; maintain healthy weight and blood pressure. Purpose. Support retinal and vascular health overall. Mechanism. Antioxidants and vascular benefits may support retinal resilience (adjunctive). NORD

  15. Smoking cessation
    Description. Structured quit plans and support. Purpose. Reduce oxidative and vascular stress that can worsen eye disease risk. Mechanism. Removes tobacco-related retinal and vascular injury drivers. NORD

  16. Digital accessibility (high-contrast, zoom, screen readers)
    Description. Use device settings and apps to enlarge text and enhance contrast. Purpose. Ease reading and device use. Mechanism. Software magnification and contrast improve legibility. NORD

  17. Psychological support
    Description. Counseling or support groups for inherited eye disease. Purpose. Reduce anxiety and improve coping. Mechanism. Education and social support improve adherence and quality of life. NORD

  18. Sun and glare control indoors
    Description. Sheers, blinds, anti-glare coatings, task lamps. Purpose. Reduce glare symptoms. Mechanism. Environmental light control lowers visual discomfort. NORD

  19. Emergency plan for acute angle-closure symptoms
    Description. Teach warning signs (sudden pain, halos, headache, nausea) and emergency pathways. Purpose. Early treatment saves vision. Mechanism. Rapid response to IOP crisis prevents nerve damage. EyeWiki

  20. Clinical-trial awareness (gene/targeted therapies)
    Description. Ask about studies for BEST1-related disease or retina gene therapy platforms. Purpose. Access emerging options under supervision. Mechanism. Investigational vectors may aim to correct RPE dysfunction; participation is voluntary and strictly regulated. NCBI

Drug treatments

Important: No drug is FDA-approved specifically for ADVIRC. Many medicines below are used to treat complications (e.g., angle-closure risk, high eye pressure, cystoid macular edema, or secondary CNV). When used for ADVIRC complications, they are often off-label. FDA labels are cited for mechanism, dose, and approved uses in related conditions.

  1. Timolol (topical beta-blocker) – IOP lowering
    Class. Beta-adrenergic antagonist. Dose/Time. Commonly 1 drop 0.25–0.5% once or twice daily per label (doctor adjusts). Purpose. Reduce high eye pressure in narrow/closed angles or secondary glaucoma risk in nanophthalmos. Mechanism. Lowers aqueous humor production at ciliary body. Side effects. Burning, dry eye; systemic beta-blocker effects (bradycardia, bronchospasm) in sensitive patients. Note. Used for glaucoma; in ADVIRC, it addresses the IOP complication. FDA Access Data+1

  2. Dorzolamide (topical carbonic anhydrase inhibitor) – IOP and macular edema adjunct
    Class. Carbonic anhydrase inhibitor (CAI). Dose/Time. Typical 1 drop 2% three times daily per label. Purpose. Lowers IOP; often used with other drops. Can also be tried off-label for cystoid macular edema (CME) in inherited retinopathies. Mechanism. Reduces aqueous production (IOP); may improve retinal fluid handling. Side effects. Bitter taste, stinging; rare corneal issues. FDA Access Data+2PMC+2

  3. Brimonidine (alpha-2 agonist) – IOP lowering
    Class. Alpha-2 adrenergic agonist. Dose/Time. 0.1–0.2% one drop three times daily per label (clinician may adjust). Purpose. Additional IOP control when angles are narrow or glaucoma risk is present. Mechanism. Lowers aqueous production and increases uveoscleral outflow. Side effects. Allergic conjunctivitis, dry mouth, fatigue. FDA Access Data+1

  4. Latanoprost (prostaglandin analog) – IOP lowering
    Class. Prostaglandin F2α analog. Dose/Time. 1 drop nightly per label. Purpose. Improve IOP control in nanophthalmos patients at glaucoma risk. Mechanism. Increases uveoscleral outflow. Side effects. Redness, iris pigment darkening, eyelash growth. FDA Access Data+1

  5. Acetazolamide (oral CAI) – IOP and off-label CME
    Class. Carbonic anhydrase inhibitor. Dose/Time. Typical 250–500 mg dosing schedules per label; clinician tailors and checks kidney/electrolytes. Purpose. Short-term IOP lowering or trial for CME in inherited retinal disease (off-label). Mechanism. Reduces aqueous formation; may reduce macular fluid in selected cases. Side effects. Paresthesias, diuresis, metabolic acidosis, kidney stone risk. FDA Access Data+1

  6. Fixed combo dorzolamide/timolol
    Class. CAI + beta-blocker. Dose/Time. 1 drop twice daily per label. Purpose. Simplify multi-drop IOP therapy. Mechanism. Dual action to reduce aqueous humor. Side effects. As per each component. FDA Access Data

  7. Ranibizumab (intravitreal anti-VEGF) – CNV complication
    Class. Anti-VEGF biologic. Dose/Time. Intravitreal injections at labeled intervals for approved retinal vascular diseases; in ADVIRC used off-label if secondary choroidal neovascularization (CNV) appears. Purpose. Treat CNV to stabilize/improve vision. Mechanism. Blocks VEGF-A to reduce leakage and neovascular growth. Side effects. Endophthalmitis risk, IOP spikes, inflammation (rare). FDA Access Data+1

  8. Aflibercept (intravitreal anti-VEGF)
    Class. VEGF-trap biologic. Dose/Time. Labeled regimens for nAMD/DME/RVO; off-label for CNV in dystrophies if present. Purpose. Control CNV leakage. Mechanism. Binds VEGF-A/B and PlGF. Side effects. Similar intravitreal risks; inflammation rare. FDA Access Data+1

  9. Dexamethasone intravitreal implant (Ozurdex) – refractory edema/uveitis
    Class. Corticosteroid implant. Dose/Time. Single-use 0.7 mg implant with labeled intervals in RVO/DME/uveitis; off-label use may be considered in stubborn edema. Purpose. Reduce retinal inflammation and fluid. Mechanism. Steroid anti-inflammatory effects lower vascular leakage. Side effects. IOP rise, cataract acceleration, infection risk. FDA Access Data+1

  10. Topical corticosteroid (short course, selected cases)
    Class. Glucocorticoid anti-inflammatory. Dose/Time. Short course under supervision. Purpose. Adjunct for rebound CME under CAI treatment in some inherited conditions. Mechanism. Reduces retinal inflammation and edema. Side effects. IOP rise, cataract with prolonged use—must be monitored. Frontiers

  11. Hyperosmotics for acute IOP spike (e.g., oral glycerol or IV mannitol)
    Class. Osmotic agents. Dose/Time. Emergency use only per physician. Purpose. Rapidly lower IOP in acute angle closure while definitive steps (e.g., laser) are arranged. Mechanism. Draw fluid from vitreous, lowering pressure. Side effects. Nausea, electrolyte shifts; IV administration risks. FDA Access Data

  12. Cycloplegic/mydriatic (peri-operative planning)
    Class. Antimuscarinic drops (e.g., atropine) under supervision. Purpose. Stabilize anterior segment in selected peri-operative plans. Mechanism. Relaxes ciliary muscle and dilates pupil. Side effects. Light sensitivity, near blur; systemic effects rare. EyeWiki

  13. Topical NSAIDs (adjunct for edema)
    Class. Non-steroidal anti-inflammatory. Purpose. Sometimes used with CAI/steroids to limit leakage. Mechanism. COX inhibition reduces prostaglandin-mediated leakage. Side effects. Surface irritation; rare corneal issues—medical supervision needed. Frontiers

  14. Carbonic anhydrase inhibitors—continuity and cycling strategy
    Description. In inherited retinal CME, long-term CAI therapy may wax and wane; clinicians sometimes cycle therapy or add steroid if “rebound” fluid occurs. Purpose. Maintain edema control with fewer side effects. Mechanism. Optimizes RPE fluid pumping and reduces leakage. Frontiers

  15. Alpha-2 agonist as adjunct (brimonidine) for neuroprotection hypothesis
    Description. Some clinicians consider alpha-2 agonists for possible neuroprotective effects in glaucoma (still debated). Purpose. Support optic nerve health when field loss risk exists. Mechanism. IOP lowering definite; neuroprotection not definitively proven. FDA Access Data

  16. Prostaglandin analog alternatives (e.g., preservative-free latanoprost)
    Description. Consider preservative-free options to improve tolerance if benzalkonium chloride sensitivity exists. Purpose. Better adherence and comfort. Mechanism. Same IOP pathway with gentler formulation. FDA Access Data

  17. Timolol gel-forming solutions
    Description. Once-daily gel can improve adherence and reduce dosing burden. Purpose. Better pressure control with simpler routine. Mechanism. Sustained ocular surface contact lowers aqueous production. FDA Access Data

  18. Fixed-combination regimens (to simplify)
    Description. Combining agents (e.g., dorzolamide/timolol) reduces bottle count and improves adherence. Purpose. Keep IOP stable in small, high-risk eyes. Mechanism. Multi-pathway IOP control in one bottle. FDA Access Data

  19. Anti-VEGF biosimilars (e.g., ranibizumab biosimilar) where available
    Description. May be used for CNV complications similarly to reference products, per label in approved indications; off-label if due to dystrophy CNV. Purpose. Improve access and reduce cost. Mechanism. VEGF inhibition reduces pathologic leakage. Safety. Same injection risks. FDA Access Data

  20. Careful peri-operative medical protocol for nanophthalmic surgery
    Description. Surgeon may pre-treat with IOP-lowering drops and anti-inflammatories; choose viscoelastics and wound plans to reduce effusion. Purpose. Prevent catastrophic choroidal/retinal events. Mechanism. Inflammation control + pressure control around surgery. EyeWiki+1

Dietary molecular supplements

  1. Lutein/zeaxanthin (macular carotenoids)
    Dose. Commonly lutein 10 mg + zeaxanthin 2 mg daily (per general eye health data). Function. Antioxidant pigments in the macula that filter blue light. Mechanism. May reduce oxidative stress in RPE/photoreceptors; adjunct only. NORD

  2. Omega-3 fatty acids (DHA/EPA)
    Dose. Typical 1 g/day combined EPA/DHA dietary intake; medical dosing varies. Function. Support retinal cell membranes and anti-inflammatory balance. Mechanism. Membrane fluidity and pro-resolving lipid mediators may aid retinal homeostasis. NORD

  3. Vitamin A within safe limits
    Dose. Do not exceed recommended intake; avoid in conditions where excess A is harmful. Function. Visual cycle support. Mechanism. Retinoid cycle co-factor; dosing must be individualized; some retinal dystrophies avoid high doses. NORD

  4. Vitamin C
    Dose. ~500 mg/day commonly used in ocular antioxidant formulas. Function. Antioxidant support. Mechanism. Scavenges free radicals; supports collagen and scleral tissue health generally. NORD

  5. Vitamin E
    Dose. As per general ocular supplement formulations. Function. Lipid-phase antioxidant. Mechanism. Protects membranes from peroxidation. NORD

  6. Zinc (with copper balance)
    Dose. Per ocular formulas (e.g., 25–80 mg zinc with copper supplement to avoid deficiency). Function. Enzyme cofactor in retinal metabolism. Mechanism. Supports antioxidant enzymes; excess can upset copper—balance is essential. NORD

  7. B-complex (B6, B9, B12) when deficient
    Dose. Correct deficiencies based on labs. Function. Lower homocysteine; nerve metabolism. Mechanism. Vascular/neurologic support that may aid overall ocular perfusion. NORD

  8. Magnesium (if low)
    Dose. Replace deficiency. Function. Vascular tone, neuromuscular support. Mechanism. May help microvascular regulation. NORD

  9. Anthocyanin-rich foods (blueberries, blackcurrants)
    Dose. Dietary. Function. Polyphenol antioxidants. Mechanism. Reduce oxidative stress; human ocular evidence is limited but safe as food. NORD

  10. General Mediterranean-style diet pattern
    Dose. Daily habit. Function. Anti-inflammatory dietary pattern. Mechanism. Improves vascular/metabolic health that indirectly supports the retina. NORD

Immunity booster / regenerative / stem-cell drugs

Important safety notice:
There are no FDA-approved systemic “immunity boosters,” regenerative drugs, or stem-cell drugs for ADVIRC or nanophthalmos. Unregulated stem-cell eye injections have caused severe harm. Any regenerative or gene-based therapy for BEST1-related disease remains investigational and should only be pursued inside registered clinical trials with ethics oversight. Below I list safer alternatives and how they work:

  1. Clinical-trial gene therapy (investigational)
    100 words. AAV-based delivery to the RPE is being studied for bestrophinopathies. Dosing, safety, and benefit are not established; availability depends on active trials. Mechanism. Replace/correct BEST1 to restore RPE chloride channel function. Dose. Trial-specific. Function. Potential disease-modifying approach (unproven). NCBI

  2. Anti-VEGF biologics (approved for other retinal diseases; off-label for dystrophy-related CNV)
    100 words. Ranibizumab/aflibercept are FDA-approved for nAMD/DME/RVO and can treat secondary CNV if it occurs in ADVIRC. Mechanism. VEGF blockade reduces leakage/new vessel growth. Dose. Intravitreal per label for approved diseases; off-label interval if used for dystrophy CNV. Function. Complication control, not gene repair. FDA Access Data+1

  3. Dexamethasone intravitreal implant (approved for RVO/DME/uveitis; off-label for stubborn edema)
    100 words. When CAIs fail, retina specialists may consider an Ozurdex implant to reduce macular fluid. Mechanism. Local steroid anti-inflammation decreases leakage. Dose. Single 0.7 mg implant; repeat per specialist. Function. Edema control while monitoring IOP and cataract risk. FDA Access Data

  4. Acetazolamide (systemic CAI) for inherited-retinal CME (off-label)
    100 words. Some case series show improved edema/vision with oral acetazolamide in inherited retinal disease. Mechanism. CAI may improve RPE fluid pumping. Dose. Physician-directed (commonly 250–500 mg schedules). Function. Symptom control; watch electrolytes and kidney function. FDA Access Data

  5. Topical dorzolamide for inherited-retinal CME (off-label)
    100 words. Multiple small studies (RP, ESCS, choroideremia) show OCT improvement with dorzolamide. Evidence is not ADVIRC-specific but physiologically related. Mechanism. CAI effect on RPE fluid transport. Dose. Often 2% three times daily. Function. Non-systemic attempt to clear cysts; monitor response. PMC+1

  6. Counseled avoidance of unapproved stem-cell injections
    100 words. Commercial “stem-cell” eye shots offered outside trials have caused permanent blindness. Mechanism. None proven; often unsafe. Dose. Not applicable. Function. Protection by not undergoing such procedures; choose regulated trials only. NCBI

Surgeries

  1. Laser peripheral iridotomy (LPI)
    Procedure. A laser creates a tiny hole in the iris to bypass pupillary block. Why. Nanophthalmic eyes have narrow angles and are prone to angle-closure; LPI reduces acute IOP spikes. EyeWiki

  2. Prophylactic scleral windows (sclerostomies) before intraocular surgery
    Procedure. Small partial-thickness scleral resections/windows (often 2–4 quadrants) are made before cataract or other surgery. Why. Thick sclera in nanophthalmos traps fluid; windows allow drainage and lower risk of uveal effusion/expulsive hemorrhage. EyeWiki

  3. Cataract extraction with special planning
    Procedure. Small-eye biometry, custom IOL power, careful wound/viscoelastic strategy, sometimes preceded by scleral windows. Why. Restore clarity while preventing choroidal effusion in a small, shallow eye. EyeWiki

  4. Surgical management of uveal effusion
    Procedure. Four-quadrant scleral windows are commonly used; vitrectomy is less helpful in nanophthalmos unless combined plans are needed. Why. To reattach retina/choroid and restore vision. Retina Today+1

  5. Glaucoma surgery (selected cases)
    Procedure. If medicines/laser fail, a specialist may consider filtering surgery or small-incision options, understanding higher choroidal effusion risk. Why. Control IOP to protect the optic nerve. EyeWiki

Preventions

  1. Regular eye checks (at least yearly). Catch glaucoma, edema, or CNV early. PubMed

  2. Know angle-closure symptoms (eye pain, halos, headache, nausea) and seek urgent care. EyeWiki

  3. Use prescribed IOP drops correctly; poor adherence raises risk. FDA Access Data

  4. Protect from UV/blue light outdoors with sunglasses/hat. NORD

  5. Manage blood pressure and diabetes to support retinal vessels. NORD

  6. Avoid smoking to lower oxidative vascular stress. NORD

  7. Discuss new systemic drugs (e.g., certain chemo) that could aggravate CME; coordinate with oncology if relevant. BioMed Central

  8. Plan surgeries in expert centers familiar with nanophthalmos. EyeWiki

  9. Maintain balanced diet (Mediterranean-style) and healthy weight. NORD

  10. Ask about clinical trials for BEST1 disease before considering any unproven “stem-cell” offers. NCBI

When to see doctors

  • Immediately for sudden eye pain, red eye, headache, halos, nausea, or sudden vision drop—these can signal acute angle-closure or uveal effusion and need urgent care. EyeWiki

  • Promptly for new distortion, central blur, or a dark spot in central vision (possible CNV or macular edema). PubMed

  • Soon if glaucoma drops cause breathing trouble, faintness, or severe fatigue—possible systemic side effects. FDA Access Data

  • Routinely every 6–12 months (or as advised) for monitoring and imaging. PubMed

What to eat and what to avoid

  • Eat: Leafy greens (spinach, kale) and colorful fruits/vegetables for carotenoids and antioxidants—good for general retinal health. NORD

  • Eat: Fish (e.g., sardines, salmon) for omega-3s; nuts and olive oil for healthy fats. NORD

  • Eat: Whole grains, legumes, and high-fiber foods to support vascular health. NORD

  • Eat: Adequate protein to support surgery recovery if needed. NORD

  • Avoid: Smoking and excessive alcohol (harm retinal/vascular health). NORD

  • Avoid: Ultra-processed, high-salt foods that can worsen blood pressure. NORD

  • Avoid: Unregulated supplements promising to “cure” genetic eye disease. NCBI

  • Consider: A daily multivitamin only if diet lacks variety; excess vitamin A is not recommended without medical advice. NORD

  • Hydrate: Keep good hydration, especially around surgery or illness, unless told otherwise by your doctor. NORD

  • Coordinate: If you have diabetes or high blood pressure, follow your medical diet plan strictly. NORD

Frequently asked questions (FAQs)

1) Is ADVIRC the same as Best disease?
No. They share the BEST1 gene, but ADVIRC shows a peripheral pigment ring and pan-retinal involvement, while Best disease mainly affects the macula. They are different points on the bestrophinopathy spectrum. NCBI

2) Can ADVIRC cause glaucoma?
People with nanophthalmos have a higher risk of angle-closure glaucoma because the front chamber is shallow and the eye is small. Pressure must be watched closely. EyeWiki

3) Will everyone with ADVIRC lose vision?
Course is often slow and variable. Some keep good vision for years; others develop macular edema, CNV, or glaucoma that need treatment. Nature+1

4) What tests confirm ADVIRC?
Exam plus imaging (OCT, autofluorescence) and BEST1 genetic testing. EOG/ERG can support the diagnosis. NCBI+1

5) Is there a cure?
No approved cure yet. Treatment targets complications and quality of life; gene therapy is under study. NCBI

6) Are there medicines for ADVIRC itself?
There is no specific approved drug. Doctors use glaucoma drops, CAIs, anti-VEGF, and steroids to treat complications (often off-label in this disease). FDA Access Data+2FDA Access Data+2

7) Do CAI drops help macular edema?
Evidence from other inherited retinopathies shows dorzolamide/acetazolamide can improve CME in some patients; response varies and can “rebound.” PMC+1

8) Why are surgeries riskier in nanophthalmos?
The sclera is thick and the eye is small, so fluid builds under the choroid easily. Scleral windows lower that risk. EyeWiki

9) Is anti-VEGF safe for ADVIRC-related CNV?
It is standard for CNV in other diseases. In dystrophy-related CNV, it is off-label but commonly used by retina specialists with similar precautions. FDA Access Data+1

10) Should my family get tested?
Because it is autosomal dominant, first-degree relatives should consider genetic counseling and eye exams. NCBI

11) Are “stem-cell” injections available?
Not as approved therapy for ADVIRC. Avoid unregulated clinics; consider clinical trials only. NCBI

12) How often should I be seen?
Usually every 6–12 months, or sooner if symptoms change, to catch treatable issues early. PubMed

13) What if I develop sudden pain and vision loss?
Go to emergency eye care—this can be angle-closure or uveal effusion needing urgent treatment. EyeWiki

14) Does diet matter?
A balanced, Mediterranean-style diet supports vascular health and general eye health; it does not cure ADVIRC. NORD

15) What is the long-term outlook?
Many patients do well with careful monitoring and timely treatment of complications. The phenotype is variable even within families. PubMed

Disclaimer: Each person’s journey is unique, treatment planlife stylefood habithormonal conditionimmune systemchronic disease condition, geological location, weather and previous medical  history is also unique. So always seek the best advice from a qualified medical professional or health care provider before trying any treatments to ensure to find out the best plan for you. This guide is for general information and educational purposes only. Regular check-ups and awareness can help to manage and prevent complications associated with these diseases conditions. If you or someone are suffering from this disease condition bookmark this website or share with someone who might find it useful! Boost your knowledge and stay ahead in your health journey. We always try to ensure that the content is regularly updated to reflect the latest medical research and treatment options. Thank you for giving your valuable time to read the article.

The article is written by Team RxHarun and reviewed by the Rx Editorial Board Members

Last Updated: October 04, 2025.

PDF Documents For This Disease Condition

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  4. National-Recommendations-for-Rare-Disease-Health-Care-Summary.[rxharun.com]
  5. History of rare diseases and their genetic.[rxharun.com]
  6. health-care-and-rare-disorders.[rxharun.com]
  7. Rare Disease Registries.[rxharun.com]
  8. autoimmune-Rare-Genetic-Diseases.[rxharun.com]
  9. Rare Genetic Diseases.[rxharun.com]
  10. rare-disease-day.[rxharun.com]
  11. Rare_Disease_Drugs_e.[rxharun.com]
  12. fda-CDER-Rare-Diseases-Public-Workshop-Master.[rxharun.com]
  13. rare-and-inherited-disease-eligibility-criteria.[rxharun.com]
  14. FDA-rare-disease-list.pdf-rxharun.com1 Human-Gene-Therapy-for-Rare Diseases_Jan_2020fda.[rxharun.com]
  15. FDA-rare-disease-lists.[rxharun.com]
  16. 30212783fnl_Rare Disease.[rxharun.com]
  17. FDA-rare-disease-list.[rxharun.com]
  18. List of rare disease.[rxharun.com]
  19. Genome Res.-2025-Steyaert-755-68.[rxharun.com]
  20. uk-practice-guidelines-for-variant-classification-v4-01-2020.[rxharun.com]
  21. PIIS2949774424010355.[rxharun.com]
  22. hidden-costs-2016.[rxharun.com]
  23. B156_CONF2-en.[rxharun.com]
  24. IRDiRC_State-of-Play-2018_Final.[rxharun.com]
  25. IRDR_2022Vol11No3_pp96_160.[rxharun.com]
  26. from-orphan-to-opportunity-mastering-rare-disease-launch-excellence.[rxharun.com]
  27. Rare disease fda.[rxharun.com]
  28. England-Rare-Diseases-Action-Plan-2022.[rxharun.com]
  29. SCRDAC 2024 Report.[rxharun.com]
  30. CORD-Rare-Disease-Survey_Full-Report_Feb-2870-2.[rxharun.com]
  31. Stats-behind-the-stories-Genetic-Alliance-UK-2024.[rxharun.com]
  32. rare-and-inherited-disease-eligibility-criteria-v2.[rxharun.com]
  33. ENG_White paper_A4_Digital_FINAL.[rxharun.com]
  34. UK_Strategy_for_Rare_Diseases.[rxharun.com]
  35. MalaysiaRareDiseaseList.[rxharun.com]
  36. EURORDISCARE_FULLBOOKr.[rxharun.com]
  37. EMHJ_1999_5_6_1104_1113.[rxharun.com]
  38. national-genomic-test-directory-rare-and-inherited-disease-eligibilitycriteria-.[rxharun.com]
  39. be-counted-052722-WEB.[rxharun.com]
  40. RDI-Resource-Map-AMR_MARCH-2024.[rxharun.com]
  41. genomic-analysis-of-rare-disease-brochure.[rxharun.com]
  42. List-of-rare-diseases.[rxharun.com]
  43. RDI-Resource-Map-AFROEMRO_APRIL[rxharun.com]
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  45. Rare disease atoz .[rxharun.com]
  46. EmanPublisher_12_5830biosciences-.[rxharun.com]

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