Ocular Tuberculosis

Earn CME/CE in your profession:

Free Review Questions

Continuing Education Activity

Ocular tuberculosis is a rare extrapulmonary manifestation of Mycobacterium tuberculosis infection. Clinical symptoms primarily occur from hematogenous dissemination from the lungs to the uveal tract. Ocular tuberculosis is a great imitator of ocular pathologies and therefore requires a high index of suspicion before making the diagnosis. This activity reviews the fundoscopic signs most closely associated with ocular tuberculosis and the management of these lesions. It highlights the role of the interprofessional team in evaluating and administering treatment, specifically in human immunodeficiency virus-infected persons, as these individuals are disproportionately affected by M. tuberculosis.

Objectives:

  • Identify the most common affected tissues of the eye.

  • Describe the characteristic fundoscopic findings and be able to differentiate them from similarly appearing diseases.

  • Describe the workup required to make a definitive or presumptive diagnosis of ocular tuberculosis.

  • Explain the importance of collaboration and coordination among the interprofessional team to enhance the delivery of care to patients affected by paradoxical worsening of symptoms after treatment initiation.

Introduction

Ocular tuberculosis is a clinical disease caused by Mycobacterium tuberculosis (TB). It has various modes of transmission, and it can infect virtually any ocular tissue. Much like the ability of syphilis to mimic various skin conditions, TB should be thought of as “the great imitator” of ocular pathologies.

Choroidal tubercles were first anatomically described in 1855 and identified with an ophthalmoscope in 1867. One year after the discovery of the organism, TB was identified in the eye in 1883.[1] An autopsy study of military TB in 1950 even reported that eye examination exceeded chest radiography in diagnostic sensitivity.[2] Since this time, TB has become increasingly rare in Western nations, and advancements in laboratory diagnostic tests have led eye examinations for choroidal tubercles to fall out of favor in recommendations and guidelines.

More than 1.7 billion people are estimated to be infected with TB. Globally, it is the leading cause of death from a single infectious agent and the leading cause of death among persons living with human immunodeficiency virus (HIV) infection.[3] It is important to recognize ocular TB as a clinical manifestation of extrapulmonary TB. A timely diagnosis can lead to early initiation of anti-tuberculosis therapy (ATT) and prevent poor patient outcomes.

Etiology

Three modes of the disease have been described for ocular tuberculosis:

  1. Direct ocular infection from an exogenous source, e.g., contact with the lids or conjunctiva (primary ocular TB).
  2. Hematogenous spread of M. tuberculosis from a pulmonary focus or extrapulmonary site (secondary ocular TB).
  3. Hypersensitivity reaction in structures of the eye after exposure to TB antigens.

The most common form of ocular involvement is hematogenous spread from pulmonary TB. Seeding may occur from primary infection or the reactivation of a dormant lesion.

M. tuberculosis spreads by aerosolized droplets. Airborne bacteria are inhaled into the respiratory alveoli, where they encounter alveolar macrophages. About 90% of these infected individuals never develop clinical disease and remain asymptomatic (latent TB). In the remaining 10%, about 5% will develop the disease within the first few years of exposure. The last 5% may develop symptoms several years later as host immunity wanes.[4]

Alveolar macrophages phagocytize the bacteria and release cytokines to recruit circulating monocytes to the site of infection, but M. tuberculosis escapes eradication by inhibiting fusion of the macrophage phagolysosome. This allows the bacteria to proliferate in nonactivated and partly-activated macrophages. Eventually, bacteria-laden macrophages disseminate into the lymphatics and venous circulation through erosions in the alveolar epithelium and migrate to oxygen-rich regions of the body, such as the lung apex, various organs, and the eye.[5]

Epidemiology

According to the World Health Organization (WHO), about 10.4 million people fall ill, and 1.8 million people die from TB each year.[6] The burden of the disease varies considerably among countries, being eight to twelve times higher in poor countries compared to industrialized countries. Geographically, the majority of TB cases in 2018 were in South-East Asia (44%), and globally the top five nations were: India (27%), China (9%), Indonesia (8%), The Philippines (6%), and Pakistan (6%). Ocular TB cases have been estimated to be under 1% in the United States, 4% in China, 6% in Italy, and 16% in Saudi Arabia.[7]

Historically, epidemiologic data of ocular TB has varied widely due to the lack of specific diagnostic criteria. In 1967, a study of 10,524 patients at a TB sanitarium reported an incidence of ocular TB in 1.4% of patients.[8] A 1997 study of 100 randomly selected Spanish TB patients reported 18% had ocular TB.[9] In patients presenting with uveitis in North India from 1996-2001, 9.86% of cases were caused by TB.[10] A prospective case series of 126 Japanese patients with uveitis from 1998-2000 reported 7.9% were due to intraocular TB.[11]

Pathophysiology

The pathophysiologic effects of Mycobacterium tuberculosis on the eye can be characterized by the mode of infection. Patients who present with extraocular involvement (lids, lacrimal apparatus, adnexa, sclera, conjunctiva, or cornea) likely have a primary ocular infection as a result of direct contact with the eye.[1][12]

Hematogenous spread of TB from pulmonary or extrapulmonary sites most commonly affects the uveal tract, consisting of the iris and ciliary body (anteriorly) and the choroid (posteriorly). Therefore, tubercular uveitis may present as anterior, intermediate, posterior, or panuveitis (granulomatous or non-granulomatous). The choroid receives the highest blood flow per unit of tissue in the body and creates an oxygen-rich environment analogous to the apex of the lung.[13] M. tuberculosis-laden macrophages deposit in the first available capillary beds upon entering the eye, which leads to posterior uveitis as the most common presentation of ocular TB. Bacilli multiply and incite local inflammation, which manifests as a choroid tubercle.[14] 

Tubercles that coalesce, or grow large, are reclassified as a tuberculoma. The tubercles and tuberculoma, involve all layers of choroidal tissue and are surrounded by obliterated choroidal blood vessels. The lesion may liquefy into a subretinal abscess. The overlying retinal pigment epithelium remains normal in early stages, but later it can become disrupted with pigmentation, and the overlying retina may detach. Early intervention may completely resolve the lesion or result in an atrophic scar.[14]

Hypersensitivity reactions involving the eye, such as phlyctenular disease or Eales disease, are theorized to be the result of an immunologic response to nonviable TB organisms in ocular tissue. The pathophysiologic mechanism is poorly understood.[15][16]

Histopathology

In most cases, the involvement of intraocular tissue makes biopsy a risky and impractical decision. In rare cases of external disease, or anterior segment involvement, a biopsy may be taken for histopathologic analysis. Presence of Ziehl-Neelson acid-fast stained bacilli and/or caseous necrosis with epithelioid cells and Langerhans giant cells suggests ocular TB. Bacteria in multinucleated giant cells are inconsistently detected by histologic staining.[16] As a result, there is extreme variability in the results and reliability of biopsies.

History and Physical

History

In recent years, those at greatest risk of developing ocular tuberculosis are immunocompromised individuals. Extrapulmonary involvement is seen in more than 50% of patients who have both acquired immunodeficiency syndrome (AIDS) and TB.[17] Others at risk include individuals on immunosuppressive therapy, healthcare workers, homeless and prisoner populations, immigrants from endemic countries, and patients with comorbid alcoholism, chronic liver disease, chronic hemodialysis, diabetes mellitus, malignancy, or silicosis.[18]

Therefore, it is crucial to complete a full past-medical and social history, and specifically inquire about the patient’s HIV status, when suspecting ocular TB. This information is especially useful when in conjunction with a history of nonspecific symptoms of pulmonary TB (chest pain, chronic cough, hemoptysis, fever, anorexia, night sweats, unexplained weight loss), travel to TB endemic country, interaction with active TB patient, prior positive radiographic findings, tuberculin skin test (TST) or interferon-gamma release assay (IGRA).

Presenting Ocular Symptoms

Ocular TB can present with any type of ocular inflammation. Patients may report acute or chronic inflammation that is unilateral or bilateral. Patients may also report headaches, flashes, floaters, or red-eye. Choroid tubercles near the macula present with diminished visual acuity and photosensitivity. Of note, the lack of visual symptoms does not rule out ocular TB as small tubercles in the peripheral fundus may be asymptomatic.[14]

Signs

Ocular TB is a great imitator of various ocular pathologies. A provider should consider many possible findings. The following are clinical signs of ocular TB described according to the anatomical location:

Extraocular TB

  • Orbit: The involvement of the orbit is most common in children.[12] Patients may present with proptosis, eyelid swelling, intermittent periorbital swelling, headache, epistaxis, decreased vision, visual field abnormalities, chemosis, Marcus Gunn pupil, epiphora, and increased orbital resistance to retropulsion.[19]
  • Eyelids: The involvement of the eyelids is also most common in children. Eyelid TB can present as lupus vulgaris with reddish-brown “apple-jelly” nodules.[20] It can also appear as a lid abscess, chronic blepharitis, or atypical chalazion.[7]
  • Lacrimal Gland: TB involvement presents as symptomatic dacryoadenitis, indistinguishable from other bacterial infections.[21]
  • Conjunctiva: Primary tuberculous conjunctivitis is a chronic disease that eventually leads to scarring. Patients present with ocular redness, discomfort, and mucopurulent discharge with regional lymphadenopathy.[22]
  • Cornea: It may present as phlyctenular keratoconjunctivitis (an inflammatory nodule at the limbus) or interstitial keratitis. The phlyctenule is believed to be a hypersensitivity reaction to TB antigen, and it may erode the epithelia and create photophobia, redness, and tearing. Tuberculous interstitial keratitis presents as a unilateral sectoral, peripheral stromal infiltrate with vascularization.[23]
  • Sclera: Tuberculous scleritis is challenging to diagnose outside the context of active systemic TB. Scleritis is usually chronic, does not respond to anti-inflammatory treatment, can be necrotizing, and usually presents anteriorly; posterior sclera involvement is rare.[24]

Intraocular TB

  • Anterior Uveitis: It is usually granulomatous, may present as iris granulomas with broad-based posterior synechiae, and Koeppe and Busacca nodules, mutton-fat keratic precipitates on the posterior aspect of the cornea, and/or complicated cataract.[25] In children, band keratopathy can occur.
  • Intermediate Uveitis: Usually presents with unilateral or bilateral asymmetry and appears similar to par planitis. Features include mild-to-moderate vitritis with snowball, snow banking, peripheral vascular sheathing, and/or peripheral retinochoroidal granulomas.[14]
  • Posterior Uveitis: It is the most common presentation of ocular TB. Common patterns include a solitary tubercle, multiple tubercles, miliary choroidal tubercles, and multifocal choroiditis (Image 1). Tubercles are white-yellow nodules that typically reside in the posterior pole. Usually, fewer than five are present but maybe as many as 50 or 60. Non-contiguous, multifocal choroiditis may progress to a diffuse, contiguous pattern called a serpiginous-like lesion. This lesion resembles serpiginous choroiditis (multifocal serpiginous choroiditis); however, in contrast to classic serpiginous choroiditis, it does not extend to the disc, tends to spare the fovea even when the macula is involved, and it is more multifocal and pigmented (Image 2). The vitreous in tuberculous serpiginous-like choroiditis is usually inflamed, whereas, in serpiginous choroiditis, there is no vitreous inflammation.[26][27]
  • Retina: TB of the retina is almost always a result of the choroidal extension. Rarely does hematogenous spread effect the retina before the choroid. Retinal lesions may take the form of either focal tubercles, subretinal abscesses, or diffuse retinitis. Occlusive retinal vasculitis may occur and induce neovascularization. Exudative retinal hemorrhagic periphlebitis with uveitis is highly suggestive of intraocular TB.[28] Gupta et al. reported about 50% of patients with tubercular retinal vasculitis to have active or healed choroiditis patches under retinal vessels. Patients may also have snowball opacities in the inferior vitreous cavity, optic disc edema, or macular star.[22]
  • Optic Nerve: Optic neuropathy develops either from direct infection induced by TB or a hypersensitivity reaction to the infectious agent. It may present as an optic nerve tubercle, papillitis, or papilledema. Optic nerve swelling and disk edema have been reported with posterior tuberculous scleritis.[29]
  • Endophthalmitis: Tubercular subretinal abscesses may burst into the vitreous cavity and present as endophthalmitis or panophthalmitis.[14]

Evaluation

Due to the various ocular tuberculosis manifestations, a clinical diagnosis is quite challenging. Developing the diagnosis of ocular TB begins with a complete history, physical exam, and fundoscopic exam. Gupta et al. identified broad-based posterior synechiae, retinal vasculitis without choroiditis, retinal vasculitis with choroiditis, and serpiginous-like choroiditis as features of ocular TB with specificities of 93%, 97%, 99%, and 98%, respectively. However, all have poor sensitivities.[28] Other highly suspicious lesions include choroidal granulomas (granulomatous uveitis), multifocal serpiginous choroiditis, occlusive retinal periphlebitis, or vasculitis.[23][24][26][27][28][29][30][31] Ocular TB should be investigated by performing the following:

  • Tuberculin skin test (TST) and/or interferon-gamma release assay (IGRA) to evaluate the cellular immune response to M. tuberculosis by the patient. Both tests have their strengths and limitations.[32] Specifically, TST can be falsely positive after BCG vaccinations and with other mycobacteria infections. Tests for IGRA, such as T-SPOT and QauntiFERON-TB Gold, are more specific, but false-positive cases can occur in low endemic areas.
  • Chest x-ray or high-resolution computed tomography (HRCT) of the chest to reveal hilar lymph node enlargement, pulmonary infiltrates, cavitation, or other signs of pulmonary TB.
  • A fine-needle aspiration biopsy or tissue biopsy attempt may be made as the culture of M. tuberculosis is the gold-standard diagnosis.[14] However, samples are difficult to collect, impose great risk on patients, and culture results may take up to 10 weeks.
  • Anterior chamber fluid or vitreous humor sample can be used in molecular diagnostic testing via polymerase chain reaction (PCR). This is becoming the method of choice because of better accuracy and rapid test results compared to culture. A case-control study of 22 patients with known TB uveitis demonstrated a 77.2% sensitivity and 92.1% specificity for PCR detection of M. tuberculosis in aqueous and vitreous aspirates.[33]
  • The WHO recommends the use of Xpert MTB/RIF assay, an automated real-time PCR, for rapid and simultaneous detection of TB and rifampicin resistance. Xpert MTB/RIF assay is currently used with sputum samples; it has not been approved by the US Food and Drug Administration for use with ocular fluids.[12][31]

A definitive diagnosis of TB uveitis is only made when M. tuberculosis, or its DNA, is isolated from ocular fluids. In most cases, ophthalmologists are unable to make a definitive diagnosis. Still, the patient may have ophthalmological features consistent with ocular TB, confirmed TB exposure (positive TST or IGRA), or evidence of a tubercular lesion on a chest x-ray or CT scan. If one of these features is present, the diagnosis of “presumed ocular TB” should be made, and treatment should be offered.[11][32][34][35] Note, a negative result for any of these tests does not rule out the disease. TSTs often yield negative results in patients with disseminated TB,[36] and about 60% of patients with extrapulmonary TB have no evidence of pulmonary TB.[37]

Treatment begins with antituberculous therapy (ATT) trial. Patients are evaluated for response to a four-drug course of isoniazid, rifampicin, ethambutol, and pyrazinamide. After 4 to 6 weeks of treatment, a positive response is taken as evidence for ocular TB, and treatment should be continued.[14]

Treatment / Management

In general, the treatment of ocular tuberculosis is the same as for pulmonary TB. Treatment consists of a four-drug regimen, administered in two phases: rifampicin, isoniazid, pyrazinamide, and ethambutol daily for two months, followed by rifampicin and isoniazid for four months. If the patient fails to respond in three to four weeks, consider multidrug resistance, TB, and management should continue in conjunction with an infectious disease specialist.

Steroids are given to reverse insult from granulomatous inflammation and to help prevent a delayed-type hypersensitivity response to TB antigens.[38] They must be used judiciously with antituberculous therapy (ATT), and not alone, as there is concern over inducing the reactivation of latent disease or prolonging the active growth of bacilli in the eye.[14] Rifampicin is an inducer of hepatic steroid metabolizing enzyme and will suppress the therapeutic effect of corticosteroids. To maintain effectiveness, it may be necessary to increase the dosage of corticosteroid when in concomitant use with rifampicin.

Paradoxical worsening after initiation of ATT has been reported. This phenomenon is thought to result from a Jarisch-Herxheimer-like reaction as the immune system gains increased exposure to bacterial antigens after treatment, and results in the release of pro-inflammatory cytokines.[39] Co-treatment with corticosteroids can circumvent this phenomenon.[14]

In addition to ATT, TB delayed hypersensitivity retinal vasculitis (Eales disease), also benefits from treatment with peripheral scatter retinal laser treatment to decrease the ischemic drive for retinal neovascularization.

Differential Diagnosis

Sarcoidosis, syphilis, toxoplasmosis, toxocariasis, and fungal infections can present as panuveitis with choroidal involvement and should be considered in the differential diagnosis of tubercular uveitis.[40] Tubercular anterior uveitis in children may mimic juvenile idiopathic uveitis.

In patients presenting predominantly with retinal vasculitis, Eales disease should be considered. Eales disease is characterized by overlapping stages of retinal vasculitis, vascular occlusion, and retinal neovascularization (Image 3). The cause of Eales disease remains unknown, but there is speculation it is a delayed retinal hypersensitivity reaction to M. tuberculosis. Prior studies have shown patients with Eales disease have consistently been found more likely to test positive for M. tuberculosis than control populations.[41]

Ophthalmologists should also consider the diagnosis of acute multifocal posterior placoid pigment epitheliopathy (AMPPPE) or classic serpiginous choroiditis in patients presenting with tuberculous serpiginous-like choroiditis. AMPPPE is a rare and poorly understood inflammatory chorioretinopathy that predominantly affects the macula. Evidence supports either a primary vasculitis or a delayed-type hypersensitivity reaction to various pathogens, including M. tuberculosis.[42] The acute phase of AMPPPE presents with multifocal flat, gray-white lesions with a placoid appearance, found at the level of the posterior pole in the retinal pigmented epithelium.[43] 

Fluorescein angiography (FA) reveals early hypofluorescence and late, irregular hyperfluorescence. Similarly, the early stages of serpiginous-like choroiditis can resemble AMPPPE as it may present with yellowish-white plaque-like lesions that appear hypofluorescent early and hyperfluorescent late on FA.[44] However, the individual discrete lesions of serpiginous-like choroiditis progressively enlarge and converge into a diffuse, contiguous choroiditis with an active leading edge.

Prognosis

The immediate use of antituberculous therapy (ATT) in ocular tuberculosis is associated with good outcomes. Most lesions completely regress and leave minimal residual damage. Depending on the severity, some lesions resolve as focal chorioretinal scars. However, lesions in the context of AIDS have been reported to progress despite ATT.[40]

Complications

It is important to be aware that ATT medications are associated with ocular adverse effects. Ethambutol causes dose-dependent ocular toxicity, e.g., optic neuritis, photophobia, extraocular muscle paresis, red-green dyschromatopsia, central scotomas, and disc edema.[45] Patients receiving doses greater than 15mg/kg/day requires an ophthalmic evaluation every four weeks. Symptoms that occur typically resolve in three to twelve months.[19]

Deterrence and Patient Education

Patients diagnosed with ocular tuberculosis should be counseled on the six-month duration of treatment and the health consequences if not completed. Directly observed treatment (DOT) is a strategy recommended by WHO to increase adherence to treatment, where a provider or family member witnesses the patient taking treatment.

Pearls and Other Issues

  • The most common form of ocular tuberculosis is from hematogenous spread.
  • Ocular TB can involve any part of the eye and can occur with or without evidence of pulmonary or extrapulmonary TB disease.
  • The most common ocular TB manifestation is granulomatous uveitis. The most common presentation is posterior uveitis.
  • The most typical lesions related to ocular TB are choroidal granulomas, occlusive retinal vasculitis, and multifocal serpiginous-like choroiditis.
  • The gold standard for diagnosis is the identification of M. tuberculosis in culture. However, this is rarely possible. PCR of ocular fluid is a recent alternative to cultures but not widely available. Diagnosis, in most cases, is “presumed ocular TB”. Ocular findings must be supported in context with risk factor history, chest radiography findings, and TST or IGRA testing. Negative tests do not rule out ocular TB.
  • Treatment of ocular TB is the same as for pulmonary TB, and concomitant steroid therapy is often required.

Enhancing Healthcare Team Outcomes

Mycobacterium tuberculosis is the top infectious disease killer of HIV/AIDS patients worldwide. In 2014, 400,000 TB-related deaths occurred among people with HIV.[6] AIDS patients are at great risk of disseminated TB, and most providers are not aware that secondary spread to ocular tissue is a potential extrapulmonary complication. A study from India analyzed 1,000 HIV patients and reported a prevalence of ocular TB in 3.8%.

M. tuberculosis was the third most common infectious opportunistic infection of the eye after cytomegalovirus retinitis and ocular toxoplasmosis in this population.[46] However, India did not include ocular TB as an extrapulmonary symptom of TB in its TB management policy documents. Eye examination was also absent from WHO diagnostic guidelines, related algorithms, and in the analysis of improving TB diagnostics.[47][48][49] 

Ophthalmologists play a special role in educating fellow providers and healthcare professionals about the possibility of ocular TB and its visual implications if gone undiagnosed. The retinal examination should be part of the basic initial workup for all patients with CD4 count less than 100 cells per µL. In HIV patients coinfected with TB, there is concern that immune reconstitution inflammatory syndrome (IRIS), worsens TB uveitis. Accordingly, in those patients, it is advisable to commence anti-TB treatment first and delay the start of highly active antiretroviral therapy (HAART) for 2-8 weeks, depending on the CD4 count.

Providers should refer TB and HIV coinfected individuals to infectious disease specialists to help manage medical treatment. Nurses and pharmacists also play a vital role in the administration of TST to HIV-infected patients. Local health officials should be contacted if an HIV patient, or any patient, tests positive for TB infection. The majority of states mandate the reporting of confirmed TB to the proper authorities within 24 hours.


(Click Image to Enlarge)
Large choroidal granuloma with subretinal fluid reaching the macula in a patient with TB choroiditis.
Large choroidal granuloma with subretinal fluid reaching the macula in a patient with TB choroiditis.
Contributed by Ahmed B. Sallam, MD, PhD, FRCOphth

(Click Image to Enlarge)
Multifocal serpiginoid choroiditis. Note the irregular multifocal pigmented choroidal lesions in the macula.
Multifocal serpiginoid choroiditis. Note the irregular multifocal pigmented choroidal lesions in the macula.
Contributed by Ahmed B. Sallam, MD, PhD, FRCOphth

(Click Image to Enlarge)
TB delayed hypersensitivity uveitis (Eales’ disease) presenting with hemorrhagic ischemic vascular occlusion
TB delayed hypersensitivity uveitis (Eales’ disease) presenting with hemorrhagic ischemic vascular occlusion. Note the retinal hemorrhages and the vascular obliteration and sheathing temporal to the macula.
Contributed by Ahmed B. Sallam, MD, PhD, FRCOphth
Details

Author

Adam J. Neuhouser

Editor:

Ahmed Sallam

Updated:

1/5/2023 1:00:30 PM

Feedback:

Send Us Your Comments

References

[1]

Helm CJ, Holland GN. Ocular tuberculosis. Survey of ophthalmology. 1993 Nov-Dec:38(3):229-56     [PubMed PMID: 8310395]

Level 3 (low-level) evidence

[2]

EMERY JL, LORBER J. Radiological and pathological correlation of miliary tuberculosis of lungs in children, with special reference to choroidal tubercles. British medical journal. 1950 Sep 23:2(4681):702-4     [PubMed PMID: 14772458]

[3]

MacNeil A, Glaziou P, Sismanidis C, Maloney S, Floyd K. Global Epidemiology of Tuberculosis and Progress Toward Achieving Global Targets - 2017. MMWR. Morbidity and mortality weekly report. 2019 Mar 22:68(11):263-266. doi: 10.15585/mmwr.mm6811a3. Epub 2019 Mar 22     [PubMed PMID: 30897077]

[4]

Dannenberg AM Jr. Delayed-type hypersensitivity and cell-mediated immunity in the pathogenesis of tuberculosis. Immunology today. 1991 Jul:12(7):228-33     [PubMed PMID: 1822092]

[5]

Krishnan N, Robertson BD, Thwaites G. The mechanisms and consequences of the extra-pulmonary dissemination of Mycobacterium tuberculosis. Tuberculosis (Edinburgh, Scotland). 2010 Nov:90(6):361-6. doi: 10.1016/j.tube.2010.08.005. Epub 2010 Sep 9     [PubMed PMID: 20829117]

[6]

Holmes KK, Bertozzi S, Bloom BR, Jha P, Bloom BR, Atun R, Cohen T, Dye C, Fraser H, Gomez GB, Knight G, Murray M, Nardell E, Rubin E, Salomon J, Vassall A, Volchenkov G, White R, Wilson D, Yadav P. Tuberculosis. Major Infectious Diseases. 2017 Nov 3:():     [PubMed PMID: 30212088]

[7]

Alvarez GG, Roth VR, Hodge W. Ocular tuberculosis: diagnostic and treatment challenges. International journal of infectious diseases : IJID : official publication of the International Society for Infectious Diseases. 2009 Jul:13(4):432-5. doi: 10.1016/j.ijid.2008.09.018. Epub 2009 Apr 22     [PubMed PMID: 19386531]

[8]

Donahue HC. Ophthalmologic experience in a tuberculosis sanatorium. American journal of ophthalmology. 1967 Oct:64(4):742-8     [PubMed PMID: 6061532]

[9]

Bouza E, Merino P, Muñoz P, Sanchez-Carrillo C, Yáñez J, Cortés C. Ocular tuberculosis. A prospective study in a general hospital. Medicine. 1997 Jan:76(1):53-61     [PubMed PMID: 9064488]

[10]

Singh R, Gupta V, Gupta A. Pattern of uveitis in a referral eye clinic in north India. Indian journal of ophthalmology. 2004 Jun:52(2):121-5     [PubMed PMID: 15283216]

[11]

Morimura Y, Okada AA, Kawahara S, Miyamoto Y, Kawai S, Hirakata A, Hida T. Tuberculin skin testing in uveitis patients and treatment of presumed intraocular tuberculosis in Japan. Ophthalmology. 2002 May:109(5):851-7     [PubMed PMID: 11986087]

[12]

Pillai S, Malone TJ, Abad JC. Orbital tuberculosis. Ophthalmic plastic and reconstructive surgery. 1995 Mar:11(1):27-31     [PubMed PMID: 7748819]

[13]

Heiden D, Saranchuk P, Keenan JD, Ford N, Lowinger A, Yen M, McCune J, Rao NA. Eye examination for early diagnosis of disseminated tuberculosis in patients with AIDS. The Lancet. Infectious diseases. 2016 Apr:16(4):493-9. doi: 10.1016/S1473-3099(15)00269-8. Epub 2016 Feb 18     [PubMed PMID: 26907735]

[14]

Gupta V, Gupta A, Rao NA. Intraocular tuberculosis--an update. Survey of ophthalmology. 2007 Nov-Dec:52(6):561-87     [PubMed PMID: 18029267]

Level 3 (low-level) evidence

[15]

Biswas J, Therese L, Madhavan HN. Use of polymerase chain reaction in detection of Mycobacterium tuberculosis complex DNA from vitreous sample of Eales' disease. The British journal of ophthalmology. 1999 Aug:83(8):994     [PubMed PMID: 10413707]

[16]

Madhavan HN, Therese KL, Gunisha P, Jayanthi U, Biswas J. Polymerase chain reaction for detection of Mycobacterium tuberculosis in epiretinal membrane in Eales' disease. Investigative ophthalmology & visual science. 2000 Mar:41(3):822-5     [PubMed PMID: 10711699]

[17]

Golden MP, Vikram HR. Extrapulmonary tuberculosis: an overview. American family physician. 2005 Nov 1:72(9):1761-8     [PubMed PMID: 16300038]

Level 3 (low-level) evidence

[18]

Khan FY. Review of literature on disseminated tuberculosis with emphasis on the focused diagnostic workup. Journal of family & community medicine. 2019 May-Aug:26(2):83-91. doi: 10.4103/jfcm.JFCM_106_18. Epub     [PubMed PMID: 31143078]

[19]

Thompson MJ, Albert DM. Ocular tuberculosis. Archives of ophthalmology (Chicago, Ill. : 1960). 2005 Jun:123(6):844-9     [PubMed PMID: 15955987]

[20]

Thomas S, Suhas S, Pai KM, Raghu AR. Lupus vulgaris--report of a case with facial involvement. British dental journal. 2005 Feb 12:198(3):135-7     [PubMed PMID: 15706374]

Level 3 (low-level) evidence

[21]

Madhukar K, Bhide M, Prasad CE, Venkatramayya. Tuberculosis of the lacrimal gland. The Journal of tropical medicine and hygiene. 1991 Jun:94(3):150-1     [PubMed PMID: 2051518]

[22]

Gupta A, Gupta V, Arora S, Dogra MR, Bambery P. PCR-positive tubercular retinal vasculitis: clinical characteristics and management. Retina (Philadelphia, Pa.). 2001:21(5):435-44     [PubMed PMID: 11642371]

[23]

Goyal JL, Jain P, Arora R, Dokania P. Ocular manifestations of tuberculosis. The Indian journal of tuberculosis. 2015 Apr:62(2):66-73. doi: 10.1016/j.ijtb.2015.04.004. Epub 2015 Jun 16     [PubMed PMID: 26117474]

[24]

Nanda M, Pflugfelder SC, Holland S. Mycobacterium tuberculosis scleritis. American journal of ophthalmology. 1989 Dec 15:108(6):736-7     [PubMed PMID: 2512813]

[25]

Tabbara KF. Ocular tuberculosis: anterior segment. International ophthalmology clinics. 2005 Spring:45(2):57-69     [PubMed PMID: 15791158]

[26]

Albert DM, Raven ML. Ocular Tuberculosis. Microbiology spectrum. 2016 Nov:4(6):. doi: 10.1128/microbiolspec.TNMI7-0001-2016. Epub     [PubMed PMID: 27837746]

[27]

Bansal R, Gupta A, Gupta V, Dogra MR, Sharma A, Bambery P. Tubercular serpiginous-like choroiditis presenting as multifocal serpiginoid choroiditis. Ophthalmology. 2012 Nov:119(11):2334-42. doi: 10.1016/j.ophtha.2012.05.034. Epub 2012 Aug 11     [PubMed PMID: 22892153]

[28]

Gupta A, Bansal R, Gupta V, Sharma A, Bambery P. Ocular signs predictive of tubercular uveitis. American journal of ophthalmology. 2010 Apr:149(4):562-70. doi: 10.1016/j.ajo.2009.11.020. Epub 2010 Feb 10     [PubMed PMID: 20149341]

[29]

MINTON J. Ocular manifestations of tuberculous meningitis: a pictorial survey. Transactions. Ophthalmological Society of the United Kingdom. 1956:76():561-79     [PubMed PMID: 13409572]

Level 3 (low-level) evidence

[30]

Gupta A, Sharma A, Bansal R, Sharma K. Classification of intraocular tuberculosis. Ocular immunology and inflammation. 2015 Feb:23(1):7-13. doi: 10.3109/09273948.2014.967358. Epub 2014 Oct 14     [PubMed PMID: 25314361]

[31]

Gupta A, Gupta V. Tubercular posterior uveitis. International ophthalmology clinics. 2005 Spring:45(2):71-88     [PubMed PMID: 15791159]

[32]

Vasconcelos-Santos DV, Zierhut M, Rao NA. Strengths and weaknesses of diagnostic tools for tuberculous uveitis. Ocular immunology and inflammation. 2009 Sep-Oct:17(5):351-5. doi: 10.3109/09273940903168688. Epub     [PubMed PMID: 19831571]

[33]

Ortega-Larrocea G, Bobadilla-del-Valle M, Ponce-de-León A, Sifuentes-Osornio J. Nested polymerase chain reaction for Mycobacterium tuberculosis DNA detection in aqueous and vitreous of patients with uveitis. Archives of medical research. 2003 Mar-Apr:34(2):116-9     [PubMed PMID: 12700006]

[34]

Figueira L, Fonseca S, Ladeira I, Duarte R. Ocular tuberculosis: Position paper on diagnosis and treatment management. Revista portuguesa de pneumologia. 2017 Jan-Feb:23(1):31-38. doi: 10.1016/j.rppnen.2016.10.004. Epub 2016 Dec 14     [PubMed PMID: 27988134]

[35]

Sanghvi C, Bell C, Woodhead M, Hardy C, Jones N. Presumed tuberculous uveitis: diagnosis, management, and outcome. Eye (London, England). 2011 Apr:25(4):475-80. doi: 10.1038/eye.2010.235. Epub 2011 Feb 4     [PubMed PMID: 21293496]

[36]

Khan FY, Aladab AH. Role of Fiberoptic Bronchoscopy in the Rapid Diagnosis of Sputum Smear-negative Disseminated Tuberculosis with Pulmonary Miliary Infiltrates. Oman medical journal. 2020 Jan:35(1):e87. doi: 10.5001/omj.2020.05. Epub 2020 Jan 15     [PubMed PMID: 31993225]

[37]

Alvarez S, McCabe WR. Extrapulmonary tuberculosis revisited: a review of experience at Boston City and other hospitals. Medicine. 1984 Jan:63(1):25-55     [PubMed PMID: 6419006]

[38]

Sharma A, Thapa B, Lavaju P. Ocular tuberculosis: an update. Nepalese journal of ophthalmology : a biannual peer-reviewed academic journal of the Nepal Ophthalmic Society : NEPJOPH. 2011 Jan-Jun:3(1):52-67. doi: 10.3126/nepjoph.v3i1.4280. Epub     [PubMed PMID: 21587325]

[39]

Ganesh SK, Abraham S, Sudharshan S. Paradoxical reactions in ocular tuberculosis. Journal of ophthalmic inflammation and infection. 2019 Sep 6:9(1):19. doi: 10.1186/s12348-019-0183-x. Epub 2019 Sep 6     [PubMed PMID: 31493128]

[40]

Griffith DE, Aksamit T, Brown-Elliott BA, Catanzaro A, Daley C, Gordin F, Holland SM, Horsburgh R, Huitt G, Iademarco MF, Iseman M, Olivier K, Ruoss S, von Reyn CF, Wallace RJ Jr, Winthrop K, ATS Mycobacterial Diseases Subcommittee, American Thoracic Society, Infectious Disease Society of America. An official ATS/IDSA statement: diagnosis, treatment, and prevention of nontuberculous mycobacterial diseases. American journal of respiratory and critical care medicine. 2007 Feb 15:175(4):367-416     [PubMed PMID: 17277290]

[41]

Madhavan HN, Therese KL, Doraiswamy K. Further investigations on the association of Mycobacterium tuberculosis with Eales' disease. Indian journal of ophthalmology. 2002 Mar:50(1):35-9     [PubMed PMID: 12090085]

[42]

Abu El-Asrar AM, Aljazairy AH. Acute posterior multifocal placoid pigment epitheliopathy with retinal vasculitis and papillitis. Eye (London, England). 2002 Sep:16(5):642-4     [PubMed PMID: 12194084]

[43]

Cozubas R, Ungureanu E, Instrate SL, Alexandrescu C, Nanu RV, Carstocea L, Voinea LM, Ciuluvica R. Similarities and differences between three different types of white dot syndrome and the therapeutic possibilities. Romanian journal of ophthalmology. 2018 Jul-Sep:62(3):183-187     [PubMed PMID: 30505986]

[44]

Gupta V, Gupta A, Arora S, Bambery P, Dogra MR, Agarwal A. Presumed tubercular serpiginouslike choroiditis: clinical presentations and management. Ophthalmology. 2003 Sep:110(9):1744-9     [PubMed PMID: 13129872]

[45]

Barron GJ, Tepper L, Iovine G. Ocular toxicity from ethambutol. American journal of ophthalmology. 1974 Feb:77(2):256-60     [PubMed PMID: 4204592]

[46]

Sudharshan S, Kaleemunnisha S, Banu AA, Shrikrishna S, George AE, Babu BR, Devaleenal B, Kumarasamy N, Biswas J. Ocular lesions in 1,000 consecutive HIV-positive patients in India: a long-term study. Journal of ophthalmic inflammation and infection. 2013 Jan 3:3(1):2. doi: 10.1186/1869-5760-3-2. Epub 2013 Jan 3     [PubMed PMID: 23514612]

[47]

Cain KP, McCarthy KD, Heilig CM, Monkongdee P, Tasaneeyapan T, Kanara N, Kimerling ME, Chheng P, Thai S, Sar B, Phanuphak P, Teeratakulpisarn N, Phanuphak N, Nguyen HD, Hoang TQ, Le HT, Varma JK. An algorithm for tuberculosis screening and diagnosis in people with HIV. The New England journal of medicine. 2010 Feb 25:362(8):707-16. doi: 10.1056/NEJMoa0907488. Epub     [PubMed PMID: 20181972]

[48]

Keeler E, Perkins MD, Small P, Hanson C, Reed S, Cunningham J, Aledort JE, Hillborne L, Rafael ME, Girosi F, Dye C. Reducing the global burden of tuberculosis: the contribution of improved diagnostics. Nature. 2006 Nov 23:444 Suppl 1():49-57     [PubMed PMID: 17159894]

[49]

Reid MJ, Shah NS. Approaches to tuberculosis screening and diagnosis in people with HIV in resource-limited settings. The Lancet. Infectious diseases. 2009 Mar:9(3):173-84. doi: 10.1016/S1473-3099(09)70043-X. Epub     [PubMed PMID: 19246021]