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XXDR-TBXXDR TB
Presenter -Dr. Nisha Singh
sir John Crofton
First to study and recognize
the importance of drug
resistance in TB.
• History
• Drug resistance type
• Mechanism of drug resistance
• Detection methods for drug resistance
• TB and HIV
• PMDT
• New Anti TB Drug
• Vaccines
Problem of TB in India (WHO SEARO
REPORT 2015-2016)
• Estimated incidence
• -2.8 MILLION CASES
o 167 (156-179) per 1 lac population annually
o 75 new smear positive PTB cases/1lakh population per year
• Estimated prevalence of TB disease
o 195 (131-271) per 1 lac population annually
• Estimated mortality
o 480,000 deaths due to TB each year
o Over 1000 deaths a day
o 2 deaths every 3 minutes
Gujarat and Maharashtra has indicated multi drug resistance levels
of 3% among new TB cases and 12-17% among previously treated
TB patients.
HISTORY
• MDR-TB was first seen in the early 90’s
• First case of XDR –TB in India was diagnosed in P. D.
Hinduja National Hospital and Medical Research Centre,
Mumbai in 2006
• In 2007 (May) – First report of two documented cases of
extremely drug resistant (XXDR) TB) in Italy
XXDR TB in India
• In January 2012 it was reported that twelve cases of TB had
been diagnosed in Mumbai which were referred to as totally
drug resistant (TDR) TB/XXDR
• NTI Bangalore confirms 8 strains to be resistance to all known
first and second line TB drugs and 2 from Mumbai were
sensitive to second line drug
• There have also been six cases in Bangalore and a further two
in New Delhi⁵
“We have little to offer these patients except for drastic surgery
and medication for some relief,”
Dr Zarir Udwadia4
Categories of Antituberculosis Drugs:
WHO
Group 1 – First-line drugs: Isoniazid, rifampicin,
ethambutol, pyrazinamide
Group 2 - Injectable agents: Kanamycin, amikacin,
capreomycin, streptomycin
Group 3 - Fluoroquinolones: Levofloxacin,
moxifloxacin, ofloxacin
Group 4 - Oral bacteriostatic agents: Ethionamide,
cycloserine, para-aminosalicylic acid (PAS),
prothionamide, terizadone
Group 5 – Unclear role: Clofazamine, linezolid,
amoxicillin/clavulanate, Imipenem/cilastatin,
thioacetazone, high-dose isoniazid, clarithromycin,
Drug resistance - types
• defined as presence of drug resistance to
one or more antiTB drugs in TB patient
who has never received prior antiTB
chemotherapy
PRIMARY
DRUG
RESISTANCE
• defined as resistance to one or more
anti TB drugs, which arises during the
course of t/t, usually as a result of non-
adherence to the recommended
regimen or faulty prescribing.
ACQUIRED
DRUG
RESISTANCE
9
Definitions of drug resistant TB
TB condition Definition
Monoresistant TB: resistant to a single drug
Polyresistant TB: resistant to at least two drugs, but not involving
Isoniazid and Rifampicin simultaneously.
Multidrug resistant (MDR) Resistance to:
+ Isoniazid
+ Rifampicin
Extensively drug
resistant (XDR)
Resistance to:
+ Isoniazid
+ Rifampicin
+ Any fluoroquinolone
+ At least one of the three injectable drugs:
capreomycin, kanamycin, amikacin
Extremely drug resistant
(XXDR)
Resistance to:
+ All first-line anti-TB drugs
+ All second-line anti-TB drugs
10
Random spontaneous mutations creating
wild TB bacteria drug-resistant
Selection of drug-resistant TB bacteria by
inadequate treatment (resulting in
monotherapy) due to:
 inadequate prescription ,supply and
intake of drugs
NATURAL
DRUG RESISTANCE
ACQUIRED
DRUG RESISTANCE
MDR /XDR/XXDR
MDR-TB can be amplified
into XDR-TB OR XXDR-TB
by:
 Inadequate/interrupted
treatment with second
line anti-TB drugs
 Indiscriminate use of
second-line drugs
 Non-adherence to
national and/or
international guidelines
Development of anti-tuberculosis drug resistance
PRIMARY
DRUG RESISTANCE
Antimycobacterial
agents
Genes involved in
resistance
Mechanism of resistance
Isoniazid i) katG (catalase
peroxidase)
i) mutations in KatG result in failure to
generate an active intermediate of INH.
ii) inh A (enoyl –ACP
reductase synthesis)
ii) overexpression of inhA allows
continuation of mycolic acid
iii) ahp C (alkyl
hydroperoxide reductase)
iii) ahpC mutations as a marker for lesions
in KatG
Rifampicin rpoB (β subunit of RNA
polymerase)
Mutations in rpoB prevent interaction with
rifampicin
Streptomycin rpsl (ribosomal protein
S12)
Mutation prevents interaction with
Streptomycin
Ethambutol EmbAB (arabinosyl
transferase)
Overexpression or mutation of embAB
allows continuation of arabinan
biosynthesis.
Pyrazinamide PncA Loss of pyrazinamidase activity results in
decreased conversion of pyrazinamide to
pyrazinoic acid, the putative active moiety
Fluoroquinolones GYra (DNA gyrase
subunit A)
Mutations in gyrA prevent interaction with
fluoroquinolones.
Mechanism of resistance of Anti-tubercular drugs
Spontaneous mutations
develop as bacilli
proliferate to >108
Drug Mutation Rate
Rifampisin 10-8
Isoniazid 10-6
Pyrazinamide 10-6
Drug resistance in XXDR
TB ³
 Atomic force microscopes confirmed morphological variation
in XXDR-TB isolates . bacilli were round , oval or even
multiple branching forms
 In addition, various type of cell division i.e., symmetrical,
asymmetrical and budding were found.
 The cell wall thicker MDR-TB isolates
 Pilli like structure that protruded from the head, tail or side
poles of the bacilli were also detected
Does HIV infection favor
TB drug resistance?
Documented evidence:
 Nosocomial transmission (HIV facilities, prisons, etc.)
 Poor adherence to TB treatment by HIV-positive patients
 Malabsorption of TB drugs (advanced
immunosuppression, chronic diarrhea)
 Acquired rifampicin resistance (diarrhea, antifungal
treatment, antiretroviral treatment)
 Poor TB programme performance (overload of TB cases
due to HIV epidemic, unknown association of HIV)
14
Phenotypic methods Genotypic methods
1. Proportion method
2. Resistance ratio method
3. Absolute concentration method
4.Colorimetric methods
5. Nitrate reductase assay
6. BACTEC TB-460
7. Mycobacterial Growth Indicator
Tube (MGIT)
8. Phage-based methods
9. E test
10. Microscopic observation
broth-drug susceptibility
assay
11. Thin-layer agar method
1. Automated DNA sequencing
2.PCR SSCP
3.Solid-phase hybridization techniques
4.Line Probe Assay
- INNO-LiPA Rif TB
- GenoType MTBDR assay
5.Rifoligotyping
6.Real Time PCR (RIF)
7.DNA Microarrays
8.Cleavage fragment length
polymorphism (CFLP)
9.Dideox fingerprinting (ddF)
10.Hybridization protection assays
(HPA)
Detection methods for resistance in TB
AUTOMATED LIQUID BASED CULTURE
BACTEC 460-TB
• Based on microbacterial metabolism
• Faster than solid culture
MB/Bact T® system
• Based on detection of CO2
• DST 8 to 12 days
BACTEC Mycobacteria Growth indicator Tube (MGIT)960
• Consumption of oxygen
• DST 8 to 12 days
ESP culture system II
Based on the detection of pressure changes
within the headspace,due to gas production
or gas consumption by microbial growth.
.
Phage Assay Methodology
• Expose strains to drug (RMP)
• Infect with D29 phage
• Grow with M.smegmatis
• Resistance correlated with plaque
formation
Microscopic Observations Drug
Susceptibility (MODS) Assay
 It is rapid drug susceptibility testing method for M.
tuberculosis (Rapid detection of MDR-TB)
 Due to faster growth of M. tuberculosis in liquid culture
characteristic cord formation observed early
 Incorporation of drugs permit concomitant DST
MOLECULAR METHODS
DNA sequencing
The Line Probe assay (LiPA) WHO
recommended
GenoType MTDBRplus
Strips (Hain Lifescience
• Most accurate and reliable method
• Detect both previously recognized
and unrecognized mutations
• For rifampicin only
• Detect rpoB mutations of rifampicin
• Can be used directly on sputum
specimens,
• Results within 1-2 days
GeneXpert MTB/RIF
PCR SSCP
• Based on property of single stranded DNA to fold into a
tertiary structure whose shape depends on it’s sequence
• Single strands of DNA differing by only one or few bases
will fold into different conformations with different
mobility's on a gel ,producing single strand conformation
polymorphism
• Detect -RIF , INH ,SM and ciprofloxacin resistance.
Microarrays
Gryadunov et al : developed a biochip for detection of
rifampicin-resistant and isoniazid-resistant strains of M.
tuberculosis .
The newest generation of TB-biochips identifies mutations
responsible for the emerging resistance of M. tuberculosis
so the highly effective second-line fluoroquinolone
antibiotics can be administered
Secondary Drugs testing: [lack of
standardized methods!]
XXDR Diagnostic
technology
CHOICE
Molecular DST (LPA
DST)
FIRST
Liquid culture isolation
and LPA DST
SECOND
Solid culture isolation
and LPA DST
THIRD
Liquid culture isolation
and Liquid DST
FOURTH
Solid culture isolation
and DST
FIFTH
New Anti TB drugs
• Bedaquiline
• Delamanid
• Pretomanid
• NC-002, NC-003
• Sutezolid
• SQ 109
• Benzothiazinones
Repurposed Anti TB drugs
• Linezolid
• Clofazamine
• Imipenem/ Meropenem
• Amoxicillin – Clavulanate
• Thioacetazone
• Clarithromycin
(Mendell, et al.Principle and Practice of INFECTIOUS DISEASES;2005:2852-
2886.)
Bedaquiline
2016 – RNTCP has
introducing BDQ
through
conditional access
programme at 6
sites in India
Programmatic Management of Drug
Resistant TB (PMDT) in India
 Efficient and timely identification of patients who require DST
 Quality-assured laboratory capacity (Smear, Culture-DST,
rapid molecular test)
 Efficient drug procurement and supply chain management
 Adherence to difficult-to-take regimens for long periods
 Prompt identification and management of side-effects
 Recording and reporting and Human and financial resources
THANK YOU
REFERENCES
• http://tbcindia.nic.in Central Tuberculosis Division, Govt Of India.
• WHO website http://www.who.int/tb/en/
• Velayati AA, et al. New insight into extremely drug-resistant
tuberculosis: using atomic force microscopy. Eur Respir J 2010;36:
1490-3.
• Udwadia, Zarir “Emergence of New Forms of Totally Drug-Resistant
Tuberculosis Bacilli”, Chest, April 6
2009 www.ncbi.nlm.nih.gov/pubmed/
• Anand, G “India in Race to Contain Untreatable Tuberculosis”, The
Wall Street Journal, 2012 //online.wsj.com/article/Mandeep Jassal,
William R Bishai. Extensively drug-resistant tuberculosis . Lancet
Infect Dis 2009; 9: 19–30
• RNTCP Briefing and Response to Dual Challenges of MDR and
XDR TB
• Topley and Wilsons Microbiology and Microbial infections
Bacteriology Vol-2,10th edition

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xxdr tb

  • 2. sir John Crofton First to study and recognize the importance of drug resistance in TB.
  • 3. • History • Drug resistance type • Mechanism of drug resistance • Detection methods for drug resistance • TB and HIV • PMDT • New Anti TB Drug • Vaccines
  • 4. Problem of TB in India (WHO SEARO REPORT 2015-2016) • Estimated incidence • -2.8 MILLION CASES o 167 (156-179) per 1 lac population annually o 75 new smear positive PTB cases/1lakh population per year • Estimated prevalence of TB disease o 195 (131-271) per 1 lac population annually • Estimated mortality o 480,000 deaths due to TB each year o Over 1000 deaths a day o 2 deaths every 3 minutes Gujarat and Maharashtra has indicated multi drug resistance levels of 3% among new TB cases and 12-17% among previously treated TB patients.
  • 5. HISTORY • MDR-TB was first seen in the early 90’s • First case of XDR –TB in India was diagnosed in P. D. Hinduja National Hospital and Medical Research Centre, Mumbai in 2006 • In 2007 (May) – First report of two documented cases of extremely drug resistant (XXDR) TB) in Italy
  • 6. XXDR TB in India • In January 2012 it was reported that twelve cases of TB had been diagnosed in Mumbai which were referred to as totally drug resistant (TDR) TB/XXDR • NTI Bangalore confirms 8 strains to be resistance to all known first and second line TB drugs and 2 from Mumbai were sensitive to second line drug • There have also been six cases in Bangalore and a further two in New Delhi⁵ “We have little to offer these patients except for drastic surgery and medication for some relief,” Dr Zarir Udwadia4
  • 7. Categories of Antituberculosis Drugs: WHO Group 1 – First-line drugs: Isoniazid, rifampicin, ethambutol, pyrazinamide Group 2 - Injectable agents: Kanamycin, amikacin, capreomycin, streptomycin Group 3 - Fluoroquinolones: Levofloxacin, moxifloxacin, ofloxacin Group 4 - Oral bacteriostatic agents: Ethionamide, cycloserine, para-aminosalicylic acid (PAS), prothionamide, terizadone Group 5 – Unclear role: Clofazamine, linezolid, amoxicillin/clavulanate, Imipenem/cilastatin, thioacetazone, high-dose isoniazid, clarithromycin,
  • 8. Drug resistance - types • defined as presence of drug resistance to one or more antiTB drugs in TB patient who has never received prior antiTB chemotherapy PRIMARY DRUG RESISTANCE • defined as resistance to one or more anti TB drugs, which arises during the course of t/t, usually as a result of non- adherence to the recommended regimen or faulty prescribing. ACQUIRED DRUG RESISTANCE
  • 9. 9 Definitions of drug resistant TB TB condition Definition Monoresistant TB: resistant to a single drug Polyresistant TB: resistant to at least two drugs, but not involving Isoniazid and Rifampicin simultaneously. Multidrug resistant (MDR) Resistance to: + Isoniazid + Rifampicin Extensively drug resistant (XDR) Resistance to: + Isoniazid + Rifampicin + Any fluoroquinolone + At least one of the three injectable drugs: capreomycin, kanamycin, amikacin Extremely drug resistant (XXDR) Resistance to: + All first-line anti-TB drugs + All second-line anti-TB drugs
  • 10. 10 Random spontaneous mutations creating wild TB bacteria drug-resistant Selection of drug-resistant TB bacteria by inadequate treatment (resulting in monotherapy) due to:  inadequate prescription ,supply and intake of drugs NATURAL DRUG RESISTANCE ACQUIRED DRUG RESISTANCE MDR /XDR/XXDR MDR-TB can be amplified into XDR-TB OR XXDR-TB by:  Inadequate/interrupted treatment with second line anti-TB drugs  Indiscriminate use of second-line drugs  Non-adherence to national and/or international guidelines Development of anti-tuberculosis drug resistance PRIMARY DRUG RESISTANCE
  • 11. Antimycobacterial agents Genes involved in resistance Mechanism of resistance Isoniazid i) katG (catalase peroxidase) i) mutations in KatG result in failure to generate an active intermediate of INH. ii) inh A (enoyl –ACP reductase synthesis) ii) overexpression of inhA allows continuation of mycolic acid iii) ahp C (alkyl hydroperoxide reductase) iii) ahpC mutations as a marker for lesions in KatG Rifampicin rpoB (β subunit of RNA polymerase) Mutations in rpoB prevent interaction with rifampicin Streptomycin rpsl (ribosomal protein S12) Mutation prevents interaction with Streptomycin Ethambutol EmbAB (arabinosyl transferase) Overexpression or mutation of embAB allows continuation of arabinan biosynthesis. Pyrazinamide PncA Loss of pyrazinamidase activity results in decreased conversion of pyrazinamide to pyrazinoic acid, the putative active moiety Fluoroquinolones GYra (DNA gyrase subunit A) Mutations in gyrA prevent interaction with fluoroquinolones. Mechanism of resistance of Anti-tubercular drugs
  • 12. Spontaneous mutations develop as bacilli proliferate to >108 Drug Mutation Rate Rifampisin 10-8 Isoniazid 10-6 Pyrazinamide 10-6
  • 13. Drug resistance in XXDR TB ³  Atomic force microscopes confirmed morphological variation in XXDR-TB isolates . bacilli were round , oval or even multiple branching forms  In addition, various type of cell division i.e., symmetrical, asymmetrical and budding were found.  The cell wall thicker MDR-TB isolates  Pilli like structure that protruded from the head, tail or side poles of the bacilli were also detected
  • 14. Does HIV infection favor TB drug resistance? Documented evidence:  Nosocomial transmission (HIV facilities, prisons, etc.)  Poor adherence to TB treatment by HIV-positive patients  Malabsorption of TB drugs (advanced immunosuppression, chronic diarrhea)  Acquired rifampicin resistance (diarrhea, antifungal treatment, antiretroviral treatment)  Poor TB programme performance (overload of TB cases due to HIV epidemic, unknown association of HIV) 14
  • 15. Phenotypic methods Genotypic methods 1. Proportion method 2. Resistance ratio method 3. Absolute concentration method 4.Colorimetric methods 5. Nitrate reductase assay 6. BACTEC TB-460 7. Mycobacterial Growth Indicator Tube (MGIT) 8. Phage-based methods 9. E test 10. Microscopic observation broth-drug susceptibility assay 11. Thin-layer agar method 1. Automated DNA sequencing 2.PCR SSCP 3.Solid-phase hybridization techniques 4.Line Probe Assay - INNO-LiPA Rif TB - GenoType MTBDR assay 5.Rifoligotyping 6.Real Time PCR (RIF) 7.DNA Microarrays 8.Cleavage fragment length polymorphism (CFLP) 9.Dideox fingerprinting (ddF) 10.Hybridization protection assays (HPA) Detection methods for resistance in TB
  • 16. AUTOMATED LIQUID BASED CULTURE BACTEC 460-TB • Based on microbacterial metabolism • Faster than solid culture MB/Bact T® system • Based on detection of CO2 • DST 8 to 12 days BACTEC Mycobacteria Growth indicator Tube (MGIT)960 • Consumption of oxygen • DST 8 to 12 days
  • 17. ESP culture system II Based on the detection of pressure changes within the headspace,due to gas production or gas consumption by microbial growth. . Phage Assay Methodology • Expose strains to drug (RMP) • Infect with D29 phage • Grow with M.smegmatis • Resistance correlated with plaque formation
  • 18. Microscopic Observations Drug Susceptibility (MODS) Assay  It is rapid drug susceptibility testing method for M. tuberculosis (Rapid detection of MDR-TB)  Due to faster growth of M. tuberculosis in liquid culture characteristic cord formation observed early  Incorporation of drugs permit concomitant DST
  • 19. MOLECULAR METHODS DNA sequencing The Line Probe assay (LiPA) WHO recommended GenoType MTDBRplus Strips (Hain Lifescience • Most accurate and reliable method • Detect both previously recognized and unrecognized mutations • For rifampicin only • Detect rpoB mutations of rifampicin • Can be used directly on sputum specimens, • Results within 1-2 days
  • 21. PCR SSCP • Based on property of single stranded DNA to fold into a tertiary structure whose shape depends on it’s sequence • Single strands of DNA differing by only one or few bases will fold into different conformations with different mobility's on a gel ,producing single strand conformation polymorphism • Detect -RIF , INH ,SM and ciprofloxacin resistance.
  • 22. Microarrays Gryadunov et al : developed a biochip for detection of rifampicin-resistant and isoniazid-resistant strains of M. tuberculosis . The newest generation of TB-biochips identifies mutations responsible for the emerging resistance of M. tuberculosis so the highly effective second-line fluoroquinolone antibiotics can be administered
  • 23. Secondary Drugs testing: [lack of standardized methods!] XXDR Diagnostic technology CHOICE Molecular DST (LPA DST) FIRST Liquid culture isolation and LPA DST SECOND Solid culture isolation and LPA DST THIRD Liquid culture isolation and Liquid DST FOURTH Solid culture isolation and DST FIFTH
  • 24. New Anti TB drugs • Bedaquiline • Delamanid • Pretomanid • NC-002, NC-003 • Sutezolid • SQ 109 • Benzothiazinones Repurposed Anti TB drugs • Linezolid • Clofazamine • Imipenem/ Meropenem • Amoxicillin – Clavulanate • Thioacetazone • Clarithromycin (Mendell, et al.Principle and Practice of INFECTIOUS DISEASES;2005:2852- 2886.) Bedaquiline 2016 – RNTCP has introducing BDQ through conditional access programme at 6 sites in India
  • 25. Programmatic Management of Drug Resistant TB (PMDT) in India  Efficient and timely identification of patients who require DST  Quality-assured laboratory capacity (Smear, Culture-DST, rapid molecular test)  Efficient drug procurement and supply chain management  Adherence to difficult-to-take regimens for long periods  Prompt identification and management of side-effects  Recording and reporting and Human and financial resources
  • 27. REFERENCES • http://tbcindia.nic.in Central Tuberculosis Division, Govt Of India. • WHO website http://www.who.int/tb/en/ • Velayati AA, et al. New insight into extremely drug-resistant tuberculosis: using atomic force microscopy. Eur Respir J 2010;36: 1490-3. • Udwadia, Zarir “Emergence of New Forms of Totally Drug-Resistant Tuberculosis Bacilli”, Chest, April 6 2009 www.ncbi.nlm.nih.gov/pubmed/ • Anand, G “India in Race to Contain Untreatable Tuberculosis”, The Wall Street Journal, 2012 //online.wsj.com/article/Mandeep Jassal, William R Bishai. Extensively drug-resistant tuberculosis . Lancet Infect Dis 2009; 9: 19–30 • RNTCP Briefing and Response to Dual Challenges of MDR and XDR TB • Topley and Wilsons Microbiology and Microbial infections Bacteriology Vol-2,10th edition