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Fixed-Dose Combinations for HIV/AIDS, Tuberculosis, and Malaria - Report of a Meeting Held 16-18 December 2003 Geneva
(2003; 199 pages)
Índice de contenido
Summary: Observations and some ways forward
A. Overall observations
B. Experiences with fixed-dose combinations
C. Public health priorities
D. IP and legal options
E. Pharmaceutical development, quality assurance, and regulatory requirements
Welcome
Objectives of the meeting
Expected outcomes
Presentations on TB FDC issues
Presentations and discussions on malaria FDC issues
Presentations and discussions concerning ARV FDCs
Presentation and discussion of cross-cutting issues related to logistics, adherence and resistance with FDCs
Procurement experiences
Intellectual property and industry issues
Regulatory issues
Concluding session
Fixed-dose combinations for tuberculosis: lessons learned from a clinical, formulation and regulatory perspective
Abstract
Tuberculosis in the world of today
Combination therapy and fixed-dose combination (FDC) formulations in the management of TB
Registration requirements for rifampicin-containing FDC formulations
Conclusions
Acknowledgments
Annex: Bioavailability of rifampicin, the Biopharmaceutic Classification System and the 4D approach to disease management
Results/c results/comments
References
Product costs of fixed-dose combination tablets in comparison with separate dispensing and or co-blistering of antituberculosis drugs
Introduction
Method
Results
Discussion
References
Fixed-dose combinations: artemisinin-based combination therapies for malaria treatment
Introduction
Background
Implementation issues
Process leading to the development of guidelines on the use of artemisinin-based combination therapies (ACTs)
Support to countries in the implementation of ACTs
Challenges/way forward
Recommendations for further research
Conclusion
References
Developing combinations of drugs for malaria examination of critical issues and lessons learnt
Background
Parasite resistance to antimalarial drugs: a major impediment to effective control
Strategies to overcome resistance
Evidence - the key to sensible recommendations
Further work on the artemisinins
Recommendations & outstanding challenges
References
Safety and long-term effectiveness of generic fixed-dose formulations of nevirapine-based HAART amongst antiretroviral-naïve HIV-infected patients in India
Abstract
Introduction
Methods
Results
Discussion
Immunological improvement
Viral load
Clinical findings
Conclusions
References
Effect of introduction of fixed-dose combinations on the drug supply chain: experiences from the field
Abstract
Introduction
Procurement
Distribution
Prescribing
Dispensing to patients
Cost to patient
Patient use
Consumption data
Conclusion
References
Effect of fixed-dose combination (FDC) medications on adherence and treatment outcomes
Introduction
Evidence of effect of FDCs or unit-of-use packaging on adherence and treatment outcomes
Research needs
Conclusion
Acknowledgements
References
Effect of fixed-dose combination (FDC) drugs on development of clinical antimicrobial resistance: a review paper
Executive summary
Introduction
Biological basis for drug resistance to anti-TB, HIV/AIDS and malaria drugs
Combination drugs in the context of AMR
Overcoming clinical resistance using combinations: what is the evidence
i
?
Future research needs
Conclusion
Selected studies comparing combinations, FDCs, blister packs and monotherapy with regard to development of antimicrobial resistance
References
Fixed-dose combination (FDC) drugs availability and use as a global public health necessity: intellectual property and other legal issues
Executive summary
Introduction
IPRs and Fixed-dose Combinations: Introduction to the “Anticommons Problem”
IPRs and Fixed-dose Combinations: The “Anticommons Problem” (II)
Overcoming IP/Legal barriers
Back to the Future: TRIPS, Public Health, Access to Medicines
Recommendations
Conclusions
References
Pharmaceutical development and quality assurance of FDCs
Abstract
Introduction
Preformulation studies
Some examples of the relevance of the properties of the API to product formulation!
Good Manufacturing Practice (GMP)
Issues that may arise in the formulation of FDCs that do not arise for single entity products include:
Changes to registered products (variations)
Quality control of FDCs
Recommendations
References
Annotated agenda
List of participants
Product costs of fixed-dose combination tablets in comparison with separate dispensing and or co-blistering of antituberculosis drugs
Robert Bwire
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Última actualización: le 24 abril 2012
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