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FUTURE RESEARCH MOVEMENT
FOR TUBERCULOSIS CONTROL
FUTURE RESEARCH MOVEMENT
FOR TUBERCULOSIS CONTROL
A/Prof. Nguyen Viet Nhung, MD., PhD
Vice director, National Lung Hospital, Hanoi, Viet Nam
Deputy Manager, National Tuberculosis control Program
Vice President, Viet Nam Association against TB and Lung Diseases
Regional Green Light Committee - WHO / WPR
Looking beyond 2015:
Rationale
At the 65th World Health Assembly in May 2012, Member States called upon WHO to
develop a new post-2015 TB strategy and targets and present this to Member States at
the 67th World Health Assembly in 2014. Some States also urged WHO to start the
formal process through the Executive Board and World Health Assembly in 2013.
Start Developing
Draft Global strategy
for TB prevention, treatment and care
post-2015
Dr Malgosia Grzemska
Stop TB Department
World Health Organization
TAG TB/WPRO
Phnom Penh, Cambodia, 23-25 October 2012
Moving towards a new approach:
Addressing the most vulnerable
Half a million women and
over 70,000 children die of
TB each year; 10 million
“TB” orphans
Poor, crowded & poorly ventilated
settings
TB linked to HIV infection, malnutrition,
alcohol, drug and tobacco use, diabetes
Half a million women and
over 70,000 children die of
TB each year; 10 million
“TB” orphans
Migrants, prisoners, minorities,
refugees face risks, discrimination
& barriers to care
Moving towards a new approach:
Addressing key challenges
Case detection
A third of cases not
diagnosed/reported
TB/HIV co infection
Special challenge in Africa
Multidrug - resistant TB
Special challenge in Eastern
Europe
Bottlenecks for financing of
research and innovation
Case detection
A third of cases not
diagnosed/reported
TB/HIV co infection
Special challenge in Africa
Multidrug - resistant TB
Special challenge in Eastern
Europe
Weak health policies,
systems, financing, and
services
Under-engaged
communities and
providers
The way forward:
Expansion with Innovation
• Greater commitment
• Active case finding
• Molecular diagnosis
• Treat all forms of TB
• Treatment of latent TB
• Research and
innovation
• Much greater engagement of
all providers and community
• Much stronger system support
• Social protection
• Whole-of-government
approach
• Major drive for Innovation
More and Better
Stop TB Strategy
• (Enhanced and)
innovative TB
care/DOTS
• Bold policies and
supportive systems
• Intensified research
and innovation
• Greater commitment
• Active case finding
• Molecular diagnosis
• Treat all forms of TB
• Treatment of latent TB
• Research and
innovation
More and
Better DOTS
• Much greater engagement of
all providers and community
• Much stronger system support
• Social protection
• Whole-of-government
approach
• Major drive for Innovation
• (Enhanced and)
innovative TB
care/DOTS
• Bold policies and
supportive systems
• Intensified research
and innovation
Post-2015
TB Strategy
Proposed three pillars
Establishing a
new post-2015 strategy
Innovativ
e TB Care
Bold
policies and
supportive
systems Intensified
research
and
innovation
WHOandPartnersSupporttocountries
Surveillance,MonitoringandEvaluation
Intensified
research
and
innovation
WHOandPartnersSupporttocountries
Surveillance,MonitoringandEvaluation
Innovative TB Care
Bold policies and
supportive systems
Intensified Research
Vision: A world free of TB
DRAFT Post-2015 TB Strategy
CORE PRINCIPLES:
Government stewardship with adequate financing
Engagement of communities and civil society; Collaboration with private sector
Promotion of human rights, ethics and equity
Adaptation of the strategy and targets at country level
Monitoring and evaluation across all strategy components
Innovative TB Care
Rapid diagnosis and systematic
screening of contacts and other
high-risk populations
Treatment of all forms of TB with
patient support
Management of drug-resistant TB,
TB/HIV and other co-morbidities
Preventive treatment of high-risk
populations
Bold policies and
supportive systems
Policies pursuing a system-wide
approach for integration of TB care in
all health services
Universal Health Coverage with free
TB care and social protection
Regulatory framework including vital
registration, mandatory case-
notification, infection control and
rational use of quality-assured drugs
Whole-of-government approach to
addressing social determinants of TB
including poverty reduction, food
security, healthy living and working
conditions
Intensified Research
Discovery, development and rapid
uptake of new diagnostics, drugs
and vaccines
Research to optimize
implementation and adopt
innovations
Sept 2012
Six categories of
TB Research
1. Epidemiology
2. Fundamental research
3. Diagnostics
4. Treatment
5. Vaccines
6. Operational and
public health research
1. Epidemiology
2. Fundamental research
3. Diagnostics
4. Treatment
5. Vaccines
6. Operational and
public health research
1. Epidemiology
– Determine the burden of TB
– Understand variations in the dynamics of TB in
different settings and identify the social and
biological drivers of M. tuberculosis transmission
at population level
2. Fundamental research
– Characterize human TB by modern biochemical,
clinical and epidemiological approaches
– Better understand the host–pathogen interaction
– Use ‘discovery science’ to identify biomarkers
that can better differentiate the stages of the
disease spectrum.
1. Epidemiology
– Determine the burden of TB
– Understand variations in the dynamics of TB in
different settings and identify the social and
biological drivers of M. tuberculosis transmission
at population level
2. Fundamental research
– Characterize human TB by modern biochemical,
clinical and epidemiological approaches
– Better understand the host–pathogen interaction
– Use ‘discovery science’ to identify biomarkers
that can better differentiate the stages of the
disease spectrum.
3. Diagnostics
– Evaluate biomarkers identified in fundamental
studies for use as diagnostic tools
– Design and validate a set of tools for diagnosis of
active drug-sensitive and drug-resistant TB and
latent TB infection that are feasible and applicable
at various health-care levels in high-burden settings
– Improve existing diagnostic tests for active drug-
sensitive and drug-resistant TB and latent TB
infection at various health-care levels in high-
burden settings
– Evaluate new diagnostic tools, and conduct
demonstration studies, followed by evaluation of
the programmatic impact of all diagnostic tools
3. Diagnostics
– Evaluate biomarkers identified in fundamental
studies for use as diagnostic tools
– Design and validate a set of tools for diagnosis of
active drug-sensitive and drug-resistant TB and
latent TB infection that are feasible and applicable
at various health-care levels in high-burden settings
– Improve existing diagnostic tests for active drug-
sensitive and drug-resistant TB and latent TB
infection at various health-care levels in high-
burden settings
– Evaluate new diagnostic tools, and conduct
demonstration studies, followed by evaluation of
the programmatic impact of all diagnostic tools
4. Treatment
– Develop new drugs and treatment strategies
– Develop a shorter regimen for drug-susceptible TB
that can be used in combination with HIV
treatment
– Develop a safer, more efficacious, shorter regimen
for drug-resistant TB that is compatible with HIV
treatment
– Develop safe, reliable, user-friendly drug regimens
suitable for all forms of TB in children and
compatible with HIV treatment
– Develop safer, more effective, shorter regimens for
TB infected individuals
– Develop safer, shorter, highly effective regimens
for drug-susceptible and drug-resistant latent TB
infection that are compatible with HIV treatment
and suitable for children
4. Treatment
– Develop new drugs and treatment strategies
– Develop a shorter regimen for drug-susceptible TB
that can be used in combination with HIV
treatment
– Develop a safer, more efficacious, shorter regimen
for drug-resistant TB that is compatible with HIV
treatment
– Develop safe, reliable, user-friendly drug regimens
suitable for all forms of TB in children and
compatible with HIV treatment
– Develop safer, more effective, shorter regimens for
TB infected individuals
– Develop safer, shorter, highly effective regimens
for drug-susceptible and drug-resistant latent TB
infection that are compatible with HIV treatment
and suitable for children
5. Vaccines
– Conduct fundamental research as a basis for the
development of effective TB vaccines
– Conduct research and clinical testing to better
understand the safety and efcacy of BCG and
candidate vaccines
– Develop standardized assays and find
biomarkers for use in clinical trials to identify
correlates of protection
– Develop new pre- and post-exposure vaccines,
new adjuvants and new delivery platforms
– Improve and standardize preclinical assays to
evaluate immunogenicity and potential
protective efcacy of new TB vaccines
– Improve and standardize testing of TB vaccines
in clinical trials
5. Vaccines
– Conduct fundamental research as a basis for the
development of effective TB vaccines
– Conduct research and clinical testing to better
understand the safety and efcacy of BCG and
candidate vaccines
– Develop standardized assays and find
biomarkers for use in clinical trials to identify
correlates of protection
– Develop new pre- and post-exposure vaccines,
new adjuvants and new delivery platforms
– Improve and standardize preclinical assays to
evaluate immunogenicity and potential
protective efcacy of new TB vaccines
– Improve and standardize testing of TB vaccines
in clinical trials
6. Operational and public health research
– Improve TB case detection and diagnosis
– Investigate methods to improve access to treatment and treatment
delivery for drug-sensitive and drug-resistant TB
– Institute sustainable collaboration with all private and public
providers of TB care and control
– Address priority operational research questions at global, regional or
national level to improve implementation of collaborative TB and
HIV activities, and also in respect of other diseases or conditions in
which the risk for TB is increased
– Design collaborative activities in other disease programmes or
situations in which TB risk is increased
– Investigate methods to encourage community participation, to
increase the effectiveness of all interventions (e.g. case-nding,
access to treatment and care delivery)
– Optimize infection control to reduce TB transmission
– Improve measurement of disease burden by effective surveillance,
monitoring and evaluation of TB programmes
– Ensure that countries have the capacity to perform TB-related
operational research to improve TB programme performance
6. Operational and public health research
– Improve TB case detection and diagnosis
– Investigate methods to improve access to treatment and treatment
delivery for drug-sensitive and drug-resistant TB
– Institute sustainable collaboration with all private and public
providers of TB care and control
– Address priority operational research questions at global, regional or
national level to improve implementation of collaborative TB and
HIV activities, and also in respect of other diseases or conditions in
which the risk for TB is increased
– Design collaborative activities in other disease programmes or
situations in which TB risk is increased
– Investigate methods to encourage community participation, to
increase the effectiveness of all interventions (e.g. case-nding,
access to treatment and care delivery)
– Optimize infection control to reduce TB transmission
– Improve measurement of disease burden by effective surveillance,
monitoring and evaluation of TB programmes
– Ensure that countries have the capacity to perform TB-related
operational research to improve TB programme performance
Five priority areas
1. Access, screening and
diagnosis of TB;
2. Sustainable collaboration with
all care-providers for TB
control;
3. Prevention of TB in people
living with HIV, and joint
treatment of HIV and TB;
4. Access to and delivery of
treatment for drug-susceptible
and M/XDR-TB;
5. Capacity-building for
operational research.
1. Access, screening and
diagnosis of TB;
2. Sustainable collaboration with
all care-providers for TB
control;
3. Prevention of TB in people
living with HIV, and joint
treatment of HIV and TB;
4. Access to and delivery of
treatment for drug-susceptible
and M/XDR-TB;
5. Capacity-building for
operational research.
KEY FACTS AND MESSAGES ON FUTURE TB RESEARCH
Global TB Report 2012 - WHO
• Develop new TB diagnostics, drugs, and vaccines
• WHO has endorsed several new diagnostic tests
or methods since 2007, including Xpert
MTB/RIF that has the potential to transform TB
care. Other new tests, including point- of- care
tests, are in development.
• 11 vaccine candidates for TB prevention in
Phase I or Phase II trials and one
immunotherapeutic vaccine in a Phase III trial. It
is hoped that one or two of the candidates in a
Phase II trial will enter a Phase III trial in the
next 2–3 years, with the possibility of licensing at
least one new vaccine by 2020.
• Develop new TB diagnostics, drugs, and vaccines
• WHO has endorsed several new diagnostic tests
or methods since 2007, including Xpert
MTB/RIF that has the potential to transform TB
care. Other new tests, including point- of- care
tests, are in development.
• 11 vaccine candidates for TB prevention in
Phase I or Phase II trials and one
immunotherapeutic vaccine in a Phase III trial. It
is hoped that one or two of the candidates in a
Phase II trial will enter a Phase III trial in the
next 2–3 years, with the possibility of licensing at
least one new vaccine by 2020.
• 11 new or repurposed anti-TB drugs in clinical trials.
– Phase III trials of 4-month regimens for the treatment of drug-
susceptible TB are expected in 2013.
– 2 new compounds are being evaluated for use as an adjunct to
current optimized regimens for MDR-TB; one compound recently
moved to a Phase III trial and the other is expected to do so before
the end of 2012.
– A new three - drug combination regimen that could be used to
treat both drug-sensitive TB and MDR-TB and shorten
treatment duration has been tested in a Phase II study of early
bactericidal activity, with encouraging results.
• Funding for TB research and development has increased in
recent years, but stagnated between 2009 and 2010. At US$
630 million in 2010, funding falls far short of the annual
target of US$ 2 billion specified in the Global Plan to Stop
TB 2011–2015.
• 11 new or repurposed anti-TB drugs in clinical trials.
– Phase III trials of 4-month regimens for the treatment of drug-
susceptible TB are expected in 2013.
– 2 new compounds are being evaluated for use as an adjunct to
current optimized regimens for MDR-TB; one compound recently
moved to a Phase III trial and the other is expected to do so before
the end of 2012.
– A new three - drug combination regimen that could be used to
treat both drug-sensitive TB and MDR-TB and shorten
treatment duration has been tested in a Phase II study of early
bactericidal activity, with encouraging results.
• Funding for TB research and development has increased in
recent years, but stagnated between 2009 and 2010. At US$
630 million in 2010, funding falls far short of the annual
target of US$ 2 billion specified in the Global Plan to Stop
TB 2011–2015.
Lead Optimization
Preclinical
Development
GLP
Tox.
Phase I Phase II Phase III
Delamanid (OPC-67683)
Gatifloxacin
Moxifloxacin
Rifapentine
AZD5847
Bedaquiline (TMC-207)
Linezolid
Novel Regimens2
PA-824
Rifapentine
SQ-109
Sutezolid (PNU-100480)
CPZEN-45
DC-159a
Q201
SQ609
SQ641
Preclinical DevelopmentDiscovery1
Clinical Development
Diarylquinoline
DprE Inhibitors
GyrB inhibitors
InhA Inhibitors
LeuRS Inhibitors
MGyrX1 inhibitors
Mycobacterial Gyrase
Inhibitors
Pyrazinamide Analogs
Riminophenazines
Ruthenium (II) complexes
Spectinamides
Translocase-1 Inhibitors
Global TB Drug Pipeline
BTZ043
TBA-354
AZD5847
Bedaquiline (TMC-207)
Linezolid
Novel Regimens2
PA-824
Rifapentine
SQ-109
Sutezolid (PNU-100480)
CPZEN-45
DC-159a
Q201
SQ609
SQ641
Diarylquinoline
DprE Inhibitors
GyrB inhibitors
InhA Inhibitors
LeuRS Inhibitors
MGyrX1 inhibitors
Mycobacterial Gyrase
Inhibitors
Pyrazinamide Analogs
Riminophenazines
Ruthenium (II) complexes
Spectinamides
Translocase-1 Inhibitors
Chemical classes: fluoroquinolone, rifamycin, oxazolidinone, nitroimidazole, diarylquinoline, benzothiazinone
1 Ongoing projects without a lead compound series can be viewed at http://www.newtbdrugs.org/pipeline-discovery.php.
2 Combination regimens: first clinical trial (NC001) of a novel TB drug regimen testing the three drug combination of PA-824,
moxifloxacin, and pyrazinamide was initiated November 2010 and completed in 2011 with promising results. The second
clinical trial (NC002) of this regimen was launched in March 2012 and will test the efficacy of the regimen in drug-sensitive
and multidrug-resistant patients. The third clinical trial (NC003) will evaluate PA-824, TMC-207, pyrazinamide and
clofazimine in combinations and is scheduled to begin September 2012.
Updated: June 18, 2012
www.newtbdrugs.org
4 Repurposed Drugs
6 New Drugs
3 New Classes
Drugs currently in the regulatory
review process
Drugs currently in the regulatory
review process
• TB Diagnosis
– Techniques
– Approach
• Treatment
– Drugs / Regimens
– Delivery Management
• Prevention
– Infection control
– Vaccination
– Preventive therapy
• Specific categories
– Smear negative
– TB/HIV
– Pediatric TB
– M/XDR TB
• Research Partnership
• TB Diagnosis
– Techniques
– Approach
• Treatment
– Drugs / Regimens
– Delivery Management
• Prevention
– Infection control
– Vaccination
– Preventive therapy
• Specific categories
– Smear negative
– TB/HIV
– Pediatric TB
– M/XDR TB
• Research Partnership
Acknowledgements
• WHO/Stop TB Department:
• Diana Elizabeth Weil, Malgosia Grzemska, Mukund Waman Uplekar
and group for developing a New TB control Strategy post 2015
• Christian Lienhardt and GROUP in development of the “An
International Roadmap for Tuberculosis Research” and “Priorities
in Operational Research to Improve Tuberculosis Care and Control”
• WHO/WPRO: Catharina Van Weezenbeek
• NTP Viet Nam: Dinh Ngoc Sy and staff
• WHO/Stop TB Department:
• Diana Elizabeth Weil, Malgosia Grzemska, Mukund Waman Uplekar
and group for developing a New TB control Strategy post 2015
• Christian Lienhardt and GROUP in development of the “An
International Roadmap for Tuberculosis Research” and “Priorities
in Operational Research to Improve Tuberculosis Care and Control”
• WHO/WPRO: Catharina Van Weezenbeek
• NTP Viet Nam: Dinh Ngoc Sy and staff
Together
for a World free of TB !
THANKS YOU
FOR YOUR ATTENTION
vietnhung@yahoo.com

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Future tb research nhung

  • 1. FUTURE RESEARCH MOVEMENT FOR TUBERCULOSIS CONTROL FUTURE RESEARCH MOVEMENT FOR TUBERCULOSIS CONTROL A/Prof. Nguyen Viet Nhung, MD., PhD Vice director, National Lung Hospital, Hanoi, Viet Nam Deputy Manager, National Tuberculosis control Program Vice President, Viet Nam Association against TB and Lung Diseases Regional Green Light Committee - WHO / WPR
  • 2.
  • 3.
  • 4. Looking beyond 2015: Rationale At the 65th World Health Assembly in May 2012, Member States called upon WHO to develop a new post-2015 TB strategy and targets and present this to Member States at the 67th World Health Assembly in 2014. Some States also urged WHO to start the formal process through the Executive Board and World Health Assembly in 2013.
  • 5. Start Developing Draft Global strategy for TB prevention, treatment and care post-2015 Dr Malgosia Grzemska Stop TB Department World Health Organization TAG TB/WPRO Phnom Penh, Cambodia, 23-25 October 2012
  • 6. Moving towards a new approach: Addressing the most vulnerable Half a million women and over 70,000 children die of TB each year; 10 million “TB” orphans Poor, crowded & poorly ventilated settings TB linked to HIV infection, malnutrition, alcohol, drug and tobacco use, diabetes Half a million women and over 70,000 children die of TB each year; 10 million “TB” orphans Migrants, prisoners, minorities, refugees face risks, discrimination & barriers to care
  • 7. Moving towards a new approach: Addressing key challenges Case detection A third of cases not diagnosed/reported TB/HIV co infection Special challenge in Africa Multidrug - resistant TB Special challenge in Eastern Europe Bottlenecks for financing of research and innovation Case detection A third of cases not diagnosed/reported TB/HIV co infection Special challenge in Africa Multidrug - resistant TB Special challenge in Eastern Europe Weak health policies, systems, financing, and services Under-engaged communities and providers
  • 8. The way forward: Expansion with Innovation • Greater commitment • Active case finding • Molecular diagnosis • Treat all forms of TB • Treatment of latent TB • Research and innovation • Much greater engagement of all providers and community • Much stronger system support • Social protection • Whole-of-government approach • Major drive for Innovation More and Better Stop TB Strategy • (Enhanced and) innovative TB care/DOTS • Bold policies and supportive systems • Intensified research and innovation • Greater commitment • Active case finding • Molecular diagnosis • Treat all forms of TB • Treatment of latent TB • Research and innovation More and Better DOTS • Much greater engagement of all providers and community • Much stronger system support • Social protection • Whole-of-government approach • Major drive for Innovation • (Enhanced and) innovative TB care/DOTS • Bold policies and supportive systems • Intensified research and innovation Post-2015 TB Strategy
  • 9. Proposed three pillars Establishing a new post-2015 strategy Innovativ e TB Care Bold policies and supportive systems Intensified research and innovation WHOandPartnersSupporttocountries Surveillance,MonitoringandEvaluation Intensified research and innovation WHOandPartnersSupporttocountries Surveillance,MonitoringandEvaluation
  • 10. Innovative TB Care Bold policies and supportive systems Intensified Research Vision: A world free of TB DRAFT Post-2015 TB Strategy CORE PRINCIPLES: Government stewardship with adequate financing Engagement of communities and civil society; Collaboration with private sector Promotion of human rights, ethics and equity Adaptation of the strategy and targets at country level Monitoring and evaluation across all strategy components Innovative TB Care Rapid diagnosis and systematic screening of contacts and other high-risk populations Treatment of all forms of TB with patient support Management of drug-resistant TB, TB/HIV and other co-morbidities Preventive treatment of high-risk populations Bold policies and supportive systems Policies pursuing a system-wide approach for integration of TB care in all health services Universal Health Coverage with free TB care and social protection Regulatory framework including vital registration, mandatory case- notification, infection control and rational use of quality-assured drugs Whole-of-government approach to addressing social determinants of TB including poverty reduction, food security, healthy living and working conditions Intensified Research Discovery, development and rapid uptake of new diagnostics, drugs and vaccines Research to optimize implementation and adopt innovations Sept 2012
  • 11. Six categories of TB Research 1. Epidemiology 2. Fundamental research 3. Diagnostics 4. Treatment 5. Vaccines 6. Operational and public health research 1. Epidemiology 2. Fundamental research 3. Diagnostics 4. Treatment 5. Vaccines 6. Operational and public health research
  • 12. 1. Epidemiology – Determine the burden of TB – Understand variations in the dynamics of TB in different settings and identify the social and biological drivers of M. tuberculosis transmission at population level 2. Fundamental research – Characterize human TB by modern biochemical, clinical and epidemiological approaches – Better understand the host–pathogen interaction – Use ‘discovery science’ to identify biomarkers that can better differentiate the stages of the disease spectrum. 1. Epidemiology – Determine the burden of TB – Understand variations in the dynamics of TB in different settings and identify the social and biological drivers of M. tuberculosis transmission at population level 2. Fundamental research – Characterize human TB by modern biochemical, clinical and epidemiological approaches – Better understand the host–pathogen interaction – Use ‘discovery science’ to identify biomarkers that can better differentiate the stages of the disease spectrum.
  • 13. 3. Diagnostics – Evaluate biomarkers identied in fundamental studies for use as diagnostic tools – Design and validate a set of tools for diagnosis of active drug-sensitive and drug-resistant TB and latent TB infection that are feasible and applicable at various health-care levels in high-burden settings – Improve existing diagnostic tests for active drug- sensitive and drug-resistant TB and latent TB infection at various health-care levels in high- burden settings – Evaluate new diagnostic tools, and conduct demonstration studies, followed by evaluation of the programmatic impact of all diagnostic tools 3. Diagnostics – Evaluate biomarkers identied in fundamental studies for use as diagnostic tools – Design and validate a set of tools for diagnosis of active drug-sensitive and drug-resistant TB and latent TB infection that are feasible and applicable at various health-care levels in high-burden settings – Improve existing diagnostic tests for active drug- sensitive and drug-resistant TB and latent TB infection at various health-care levels in high- burden settings – Evaluate new diagnostic tools, and conduct demonstration studies, followed by evaluation of the programmatic impact of all diagnostic tools
  • 14. 4. Treatment – Develop new drugs and treatment strategies – Develop a shorter regimen for drug-susceptible TB that can be used in combination with HIV treatment – Develop a safer, more efcacious, shorter regimen for drug-resistant TB that is compatible with HIV treatment – Develop safe, reliable, user-friendly drug regimens suitable for all forms of TB in children and compatible with HIV treatment – Develop safer, more effective, shorter regimens for TB infected individuals – Develop safer, shorter, highly effective regimens for drug-susceptible and drug-resistant latent TB infection that are compatible with HIV treatment and suitable for children 4. Treatment – Develop new drugs and treatment strategies – Develop a shorter regimen for drug-susceptible TB that can be used in combination with HIV treatment – Develop a safer, more efcacious, shorter regimen for drug-resistant TB that is compatible with HIV treatment – Develop safe, reliable, user-friendly drug regimens suitable for all forms of TB in children and compatible with HIV treatment – Develop safer, more effective, shorter regimens for TB infected individuals – Develop safer, shorter, highly effective regimens for drug-susceptible and drug-resistant latent TB infection that are compatible with HIV treatment and suitable for children
  • 15. 5. Vaccines – Conduct fundamental research as a basis for the development of effective TB vaccines – Conduct research and clinical testing to better understand the safety and efcacy of BCG and candidate vaccines – Develop standardized assays and nd biomarkers for use in clinical trials to identify correlates of protection – Develop new pre- and post-exposure vaccines, new adjuvants and new delivery platforms – Improve and standardize preclinical assays to evaluate immunogenicity and potential protective efcacy of new TB vaccines – Improve and standardize testing of TB vaccines in clinical trials 5. Vaccines – Conduct fundamental research as a basis for the development of effective TB vaccines – Conduct research and clinical testing to better understand the safety and efcacy of BCG and candidate vaccines – Develop standardized assays and nd biomarkers for use in clinical trials to identify correlates of protection – Develop new pre- and post-exposure vaccines, new adjuvants and new delivery platforms – Improve and standardize preclinical assays to evaluate immunogenicity and potential protective efcacy of new TB vaccines – Improve and standardize testing of TB vaccines in clinical trials
  • 16. 6. Operational and public health research – Improve TB case detection and diagnosis – Investigate methods to improve access to treatment and treatment delivery for drug-sensitive and drug-resistant TB – Institute sustainable collaboration with all private and public providers of TB care and control – Address priority operational research questions at global, regional or national level to improve implementation of collaborative TB and HIV activities, and also in respect of other diseases or conditions in which the risk for TB is increased – Design collaborative activities in other disease programmes or situations in which TB risk is increased – Investigate methods to encourage community participation, to increase the effectiveness of all interventions (e.g. case-nding, access to treatment and care delivery) – Optimize infection control to reduce TB transmission – Improve measurement of disease burden by effective surveillance, monitoring and evaluation of TB programmes – Ensure that countries have the capacity to perform TB-related operational research to improve TB programme performance 6. Operational and public health research – Improve TB case detection and diagnosis – Investigate methods to improve access to treatment and treatment delivery for drug-sensitive and drug-resistant TB – Institute sustainable collaboration with all private and public providers of TB care and control – Address priority operational research questions at global, regional or national level to improve implementation of collaborative TB and HIV activities, and also in respect of other diseases or conditions in which the risk for TB is increased – Design collaborative activities in other disease programmes or situations in which TB risk is increased – Investigate methods to encourage community participation, to increase the effectiveness of all interventions (e.g. case-nding, access to treatment and care delivery) – Optimize infection control to reduce TB transmission – Improve measurement of disease burden by effective surveillance, monitoring and evaluation of TB programmes – Ensure that countries have the capacity to perform TB-related operational research to improve TB programme performance
  • 17. Five priority areas 1. Access, screening and diagnosis of TB; 2. Sustainable collaboration with all care-providers for TB control; 3. Prevention of TB in people living with HIV, and joint treatment of HIV and TB; 4. Access to and delivery of treatment for drug-susceptible and M/XDR-TB; 5. Capacity-building for operational research. 1. Access, screening and diagnosis of TB; 2. Sustainable collaboration with all care-providers for TB control; 3. Prevention of TB in people living with HIV, and joint treatment of HIV and TB; 4. Access to and delivery of treatment for drug-susceptible and M/XDR-TB; 5. Capacity-building for operational research.
  • 18. KEY FACTS AND MESSAGES ON FUTURE TB RESEARCH Global TB Report 2012 - WHO • Develop new TB diagnostics, drugs, and vaccines • WHO has endorsed several new diagnostic tests or methods since 2007, including Xpert MTB/RIF that has the potential to transform TB care. Other new tests, including point- of- care tests, are in development. • 11 vaccine candidates for TB prevention in Phase I or Phase II trials and one immunotherapeutic vaccine in a Phase III trial. It is hoped that one or two of the candidates in a Phase II trial will enter a Phase III trial in the next 2–3 years, with the possibility of licensing at least one new vaccine by 2020. • Develop new TB diagnostics, drugs, and vaccines • WHO has endorsed several new diagnostic tests or methods since 2007, including Xpert MTB/RIF that has the potential to transform TB care. Other new tests, including point- of- care tests, are in development. • 11 vaccine candidates for TB prevention in Phase I or Phase II trials and one immunotherapeutic vaccine in a Phase III trial. It is hoped that one or two of the candidates in a Phase II trial will enter a Phase III trial in the next 2–3 years, with the possibility of licensing at least one new vaccine by 2020.
  • 19.
  • 20. • 11 new or repurposed anti-TB drugs in clinical trials. – Phase III trials of 4-month regimens for the treatment of drug- susceptible TB are expected in 2013. – 2 new compounds are being evaluated for use as an adjunct to current optimized regimens for MDR-TB; one compound recently moved to a Phase III trial and the other is expected to do so before the end of 2012. – A new three - drug combination regimen that could be used to treat both drug-sensitive TB and MDR-TB and shorten treatment duration has been tested in a Phase II study of early bactericidal activity, with encouraging results. • Funding for TB research and development has increased in recent years, but stagnated between 2009 and 2010. At US$ 630 million in 2010, funding falls far short of the annual target of US$ 2 billion specified in the Global Plan to Stop TB 2011–2015. • 11 new or repurposed anti-TB drugs in clinical trials. – Phase III trials of 4-month regimens for the treatment of drug- susceptible TB are expected in 2013. – 2 new compounds are being evaluated for use as an adjunct to current optimized regimens for MDR-TB; one compound recently moved to a Phase III trial and the other is expected to do so before the end of 2012. – A new three - drug combination regimen that could be used to treat both drug-sensitive TB and MDR-TB and shorten treatment duration has been tested in a Phase II study of early bactericidal activity, with encouraging results. • Funding for TB research and development has increased in recent years, but stagnated between 2009 and 2010. At US$ 630 million in 2010, funding falls far short of the annual target of US$ 2 billion specified in the Global Plan to Stop TB 2011–2015.
  • 21. Lead Optimization Preclinical Development GLP Tox. Phase I Phase II Phase III Delamanid (OPC-67683) Gatifloxacin Moxifloxacin Rifapentine AZD5847 Bedaquiline (TMC-207) Linezolid Novel Regimens2 PA-824 Rifapentine SQ-109 Sutezolid (PNU-100480) CPZEN-45 DC-159a Q201 SQ609 SQ641 Preclinical DevelopmentDiscovery1 Clinical Development Diarylquinoline DprE Inhibitors GyrB inhibitors InhA Inhibitors LeuRS Inhibitors MGyrX1 inhibitors Mycobacterial Gyrase Inhibitors Pyrazinamide Analogs Riminophenazines Ruthenium (II) complexes Spectinamides Translocase-1 Inhibitors Global TB Drug Pipeline BTZ043 TBA-354 AZD5847 Bedaquiline (TMC-207) Linezolid Novel Regimens2 PA-824 Rifapentine SQ-109 Sutezolid (PNU-100480) CPZEN-45 DC-159a Q201 SQ609 SQ641 Diarylquinoline DprE Inhibitors GyrB inhibitors InhA Inhibitors LeuRS Inhibitors MGyrX1 inhibitors Mycobacterial Gyrase Inhibitors Pyrazinamide Analogs Riminophenazines Ruthenium (II) complexes Spectinamides Translocase-1 Inhibitors Chemical classes: fluoroquinolone, rifamycin, oxazolidinone, nitroimidazole, diarylquinoline, benzothiazinone 1 Ongoing projects without a lead compound series can be viewed at http://www.newtbdrugs.org/pipeline-discovery.php. 2 Combination regimens: first clinical trial (NC001) of a novel TB drug regimen testing the three drug combination of PA-824, moxifloxacin, and pyrazinamide was initiated November 2010 and completed in 2011 with promising results. The second clinical trial (NC002) of this regimen was launched in March 2012 and will test the efficacy of the regimen in drug-sensitive and multidrug-resistant patients. The third clinical trial (NC003) will evaluate PA-824, TMC-207, pyrazinamide and clofazimine in combinations and is scheduled to begin September 2012. Updated: June 18, 2012 www.newtbdrugs.org 4 Repurposed Drugs 6 New Drugs 3 New Classes Drugs currently in the regulatory review process Drugs currently in the regulatory review process
  • 22.
  • 23. • TB Diagnosis – Techniques – Approach • Treatment – Drugs / Regimens – Delivery Management • Prevention – Infection control – Vaccination – Preventive therapy • Specific categories – Smear negative – TB/HIV – Pediatric TB – M/XDR TB • Research Partnership • TB Diagnosis – Techniques – Approach • Treatment – Drugs / Regimens – Delivery Management • Prevention – Infection control – Vaccination – Preventive therapy • Specific categories – Smear negative – TB/HIV – Pediatric TB – M/XDR TB • Research Partnership
  • 24. Acknowledgements • WHO/Stop TB Department: • Diana Elizabeth Weil, Malgosia Grzemska, Mukund Waman Uplekar and group for developing a New TB control Strategy post 2015 • Christian Lienhardt and GROUP in development of the “An International Roadmap for Tuberculosis Research” and “Priorities in Operational Research to Improve Tuberculosis Care and Control” • WHO/WPRO: Catharina Van Weezenbeek • NTP Viet Nam: Dinh Ngoc Sy and staff • WHO/Stop TB Department: • Diana Elizabeth Weil, Malgosia Grzemska, Mukund Waman Uplekar and group for developing a New TB control Strategy post 2015 • Christian Lienhardt and GROUP in development of the “An International Roadmap for Tuberculosis Research” and “Priorities in Operational Research to Improve Tuberculosis Care and Control” • WHO/WPRO: Catharina Van Weezenbeek • NTP Viet Nam: Dinh Ngoc Sy and staff
  • 25. Together for a World free of TB ! THANKS YOU FOR YOUR ATTENTION vietnhung@yahoo.com