Treatment of Latent TB Infection (LTBI)

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Transcription:

Treatment of Latent TB Infection (LTBI) Mahesh C. Patel, MD June 14, 2017 2014 MFMER slide-1

Mahesh C. Patel, MD Associate Professor Treatment of LTBI Department of Internal Medicine, Division of Infectious Diseases University of Illinois at Chicago 2014 MFMER slide-2

DISCLOSURE NO relevant financial relationships NO conflicts of interest 2014 MFMER slide-3

OBJECTIVES Describe the current guidelines for LTBI treatment Describe monitoring recommendations for patients on LTBI treatment 2014 MFMER slide-4

DEFINITION Latent TB Infection is INFECTION and NOT DISEASE Suppressed by host defenses Goal should be to identify and treat those with LTBI to reduce risk of reactivation 2014 MFMER slide-5

Source: WHO 2014 MFMER slide-6

Factors to Consider when Choosing a Regimen Drug-susceptibility of presumed source case Coexisting medical conditions Potential for drug-drug interactions Patients in whom adherence is questionable, consider DOT 2014 MFMER slide-7

Isoniazid (INH) 6 month 9 month TREATMENT REGIMENS INH and Rifapentine (RPT) 12 doses, once weekly Rifampin x 4 months (INH and Rifampin x 3 months) Limited data in HIV-UNinfected persons Consider if DOT or RPT not available 2014 MFMER slide-8

INH Therapy Bulletin of the World Health Organization, 60: (4): 555-564 (1982) 2014 MFMER slide-9

INH Therapy Bulletin of the World Health Organization, 60: (4): 555-564 (1982) 2014 MFMER slide-10

Isoniazid 12 months is probably more efficacious than 6 months BUT, 6 months has greater adherence and may be more cost effective (and less hepatotoxic) So after extrapolation of this and other trials/data, 9 months was chosen The International Journal of Tuberculosis and Lung Disease, Volume 3, Number 10, October 1999, pp. 847-850(4) 2014 MFMER slide-11

INH Issues Hepatitis: 0.5 to 1 % (fatal in ~ 0.1 %) Risk factors: Increased age, alcohol consumption, underlying liver disease, concurrent use of hepatotoxic agents,? Viral hepatitis, pregnancy, female gender, IVDU Asymptomatic elevation in LFTs in 10-20%. Hold if LFTs > 3 x ULN with symptoms or > 5 x ULN if asymptomatic Peripheral neuropathy: 0.2% risk Interferes with metabolism of pyridoxine, so can be prevented with pyridoxine therapy Only recommended if other condition associated with neuropathy like DM, HIV, CKD, EtOHism, pregnancy/breastfeeding 2014 MFMER slide-12

INH Hepatotoxicity INT J TUBERC LUNG DIS 14(11):1374 1381 2014 MFMER slide-13

4 months of therapy Rifampin Ideally to be used in those who cannot tolerate INH Reduction in TB incidence similar to INH Low rate of hepatotoxicity and well-tolerated ISSUES: Drug-drug interactions (therefore, be aware in HIV patients on ARVs) Pruritis/Rash in ~ 6 % Hepatotoxicity in 0.6% 2014 MFMER slide-14

INH and Rifapentine (RPT) 12 Dose 12-dose once-weekly regimen of INH and RPT = 9 months of INH NOT recommended: Children < 2 yo HIV/AIDS on ARVs INH or rifampin-resistant MTb Pregnant women (or those expecting to become pregnant) 2014 MFMER slide-15

INH and RPT Side Effects Hepatotoxicity greater in INH only group vs. this combo group, but hypersensitivity more frequent in combo group Combo therapy also associated with flu-like syndrome and systemic drug reaction (~ 3.5%) 2014 MFMER slide-16

Special Groups Contacts of patients with TB Exposed to INH-resistant TB: Use RIF Exposed to MDR TB: Consult expert If previously treated, likely do not need retreatment (except for high risk individuals such as young children and immunosuppressed persons) 2014 MFMER slide-17

Special Groups (continued) HIV-infected persons INH x 9 months is gold standard if receiving ARVs Substitute Rifabutin for Rifampin in patients on certain ARVs HIV positive NOT on ARTx can be given 12- dose regimen of INH/RPT May consider treatment of HIV-infected persons with recent exposure to TB even if TB test is negative 2014 MFMER slide-18

Special Groups (continued) IMMEDIATE treatment of LTBI if HIV-infected or a recent contact Delay therapy about 2-3 months post delivery if without other risk factors INH daily or twice weekly DOT is preferred (with pyridoxine) NO 12-dose regimen Increased risk of hepatotoxicity OK to breastfeed 2014 MFMER slide-19

Monitoring of patients Monthly visit EDUCATION!! Signs of hepatitis Adherence to meds Drug side effects (eg fever, anorexia, icterus, rash, n/v, RUQ abdominal pain) LAB TESTING Baseline labs NOT routinely necessary Obtain in patients with liver disease, HIV, pregnancy, hx of liver disease, EtOH users. Potentially for those on other liver meds Test symptomatic individuals 2014 MFMER slide-20

Address adherence Adherence EDUCATION: Why are they taking INH?? If issues, collaborate with local health dept DOT if high risk Case management Free/Low-cost meds 2014 MFMER slide-21

WHAT TO DO IF THERAPY IS INTERRUPTED? Who knows?? INH regimen (6 or 9 months) If LESS than three months have been missed, probably can RESUME where left off If MORE than three months have been missed, RESTART therapy Rifampin Regimen (3 or 4 months) If LESS then two months have been missed, probably can RESUME where left off If MORE than two months have been missed, RESTART therapy 2014 MFMER slide-22

Post-Treatment Follow-Up Provide patient with documentation of IGRA/TST, CXR results, medication name and duration of RX Discuss signs/symptoms of TB disease (remember, risk decreases by 60-90% after completion of therapy) REPEAT CXRs NOT NEEDED unless patient has signs/symptoms of TB disease (even if patient does NOT complete therapy) 2014 MFMER slide-23

OBJECTIVES Describe the current guidelines for LTBI treatment Describe monitoring recommendations for patients on LTBI treatment 2014 MFMER slide-24

QUESTION Which of the following is most concerning when using Rifampin? a)hepatotoxicity b)drug-drug interactions c) Bone Marrow Suppression d)acute Kidney Injury e)neutropenia 2014 MFMER slide-25

Question INH and Rifapentine 12 dose therapy for LTBI is most appropriate for which of the following patients? a) 18 month old boy exposed to INH sensitive tuberculosis who now has a PPD skin test showing 22 mm of induration. b) A pregnant female with a new positive PPD at 34 weeks gestation c) An asymptomatic HIV positive patient who is wellcontrolled on his current antiretroviral regimen with a new positive PPD skin test d) A 42 y/o female with insulin-requiring diabetes mellitus e) A 24 y/o male medical student exposed to a patient in the hospital with possible rifampin-resistant TB 2014 MFMER slide-26

Questions/Comments?? Contact Information Mahesh C. Patel, M.D. Office: 312-996-6732 Cell: 917-721-5281 Email: mp3@uic.edu 2014 MFMER slide-27

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