1. A seminar on Recent advancement in impurity profiling Presented by Sudipkumar modh 1

2. Agenda 2 1. Definition of ICH 2. Importance 3. History 4. Systemic approach 5.Isolation And Identification 6.Case study 7.Methodology a)Classical approaches b)Modern approaches 8.Conclusion

4. Detection, identification/structureelucidation

5. Quantitative determination

6. Of organic and inorganic impurities and residual solvents in bulk drugs & pharmaceutical formulations3

7. Importance all phases of synthetic drug research and production from the gram scale preparation of new compounds For pharmacological screening up to the scaling up procedure and finally the production of bulk drugs Differentiate between synthesis-related impurities and degradation products 4

8. HISTORY of instrumental analysis Period following world war II,rapid development of pharmaceutical industry Instrumental analysis was developed with military technology Qualitative analysis was met by molecular spectroscopy but with complexity Spectroscopic method were generally complex, and there was a need of expert spectroscopist Separations techniques came, at the end of 19th century revolution came by development of TLC After world war II,GC developed and HPLC after two decades The fully Instrumental technique science arrived 5

9. Systemic approach According to ICH Q3A(R2) 6 Maximum Reporting Identification Qualification daily dose threshold threshold threshold (g/day) (%)

10. Systemic approach 7

12. 2nd determine fragmentation pathway from MS/MS data Empirical formula of HRMS is useful, if impurity is unknown and unrelated with drug In this case, by FT-IR,FT-Raman or both, functional groups are identified Structure is eluted by MS and NMR (Homo and hetero nuclear direct and long range chemical shift correlation experiments) 8

14. Supercritical fluid chromatography

15. Gas chromatography

20. DEPT

21. INEPT

22. 2d NMR like

23. COSY

24. TOCSY

25. HSQC

26. HMBCAre used now a days 11 HSQC (Heteronuclear Single Quantum Coherence) HMBC (Heteronuclear Multiple Bond Coherence) Distortion less Enhancement by Polarization Transfer(DEPT) Insensitive Nuclei Enhanced by Polarization Transfer (INEPT)

28. Case study Isolation And Identification Characterization of an unstable process impurity in the protease inhibitor Tipranavir Colored contaminant was being formed in final step of the synthetic process Formed due to coupling of aniline-like derivative with pyridine being used as acid scavenger Isolated by methanol stripping of silica gel chromatography methanol solution containing the colored impurity was bright red half life of about 18 h in methanol and <10 min in acetone By 1.7-mm 600-MHz SMIDG probe, sample was prepared and data set consisting of a proton reference spectrum, TOCSY, HSQC, and 10-Hz optimized HMBC spectra was acquired 13 SMIDG=sub micro-inverse-detection gradient

29. Characterization of an unstable process impurity in the protease inhibitor Tipranavir Case study Isolation And Identification drug Formed colored impurity 14 Starting material

31. 7.82(t)

32. 6.27(t)The doublet (8.25) and one of the triplets (6.27 ppm) , twice the intensity of triplet (7.82 ppm), which had an integrated intensity corresponding to half of that of a one proton signal in the drug molecule. Conclusion: impurity contained two molecules of drug and that the new resonances were present in a ratio of 2 : 2 : 1 The TOCSY spectrum confirmed the coupling of the new resonances in the aromatic region Isolation And Identification Case study Characterization of an unstable process impurity in the protease inhibitor Tipranavir 15

33. A HRMS spectrum gave exact mass of 848.47287Da (less the ionizing proton) corresponding to the molecular weight of two of the aniline precursor molecules and a C5H5 fragment consistent with the integration of the new aromatic resonances in proton spectrum. GHSQC data established the following direct proton– carbon correlation: 8.25/152.7, 7.82/125.8, and 6.27/106.2 ppm HMBC correlations linked at 8.25/152.7 ppm resonant pair to aromatic quaternary carbon bearing aniline group resonating at 142.6 ppm. other correlations were internal to five-carbon fragment Isolation And Identification Case study Characterization of an unstable process impurity in the protease inhibitor Tipranavir 16

34. Isolation And Identification HSQC spectrum Case study Characterization of an unstable process impurity in the protease inhibitor Tipranavir 17

35. Isolation And Identification HMBC spectrum Case study Characterization of an unstable process impurity in the protease inhibitor Tipranavir 18

38. separation and determination of impurities with known structure

39. Isolation of the impurity and off-line structure elucidation

40. Modern approach

41. Using on-line hyphenated separation/spectroscopic methods20

43. Capillary Electrophoresis

45. HPLC HPLC is often used with UV Chemometric methods used for separation optimisation but also for improving quantitative analysis Dimension 150-250 x 4.0-4.6 mm RP-stationary phase with particle size of 3.5-5.0 μm Rt in range of 10-20 min Ultra-performance liquid chromatography (UPLC) uses short and narrow-bore columns with small particle size packing Exp Impurities of primaquine phosphate dimensions of the column were 50 x 2.1mm C18 silica packing and 1.7 μm separation was achieved within 2 minutes Classical approach…. 22

46. A new development in RP-HPLC is the introduction of oil-in-water emulsion into the mobile phase This method, named micro emulsion liquid chromatography (MELC) special application in field of impurity profiling by HPLC is high-speed counter-current chromatography (HSCCC) (semi)preparative Analysis by HPLC-DAD to determine relative purities of each fraction in course of the preparative isolation of drugs from e.g. medicinal plant matrices 23 HPLC Classical approach….

50. An example is the polarographic and UV methods

51. Exp Determination of benzophenone impurity in phenytoin impurities

52. and low concentration of phenytoin do not allow direct use of UV spectrophotometry in drug impurity profiling

53. UV Derivative spectrophotometry is advantageous

54. Used in drug degradation studies where the relative concentration of the degradants is in per cent range

55. Exp Determination of omeprazole sulphone in omeprazole

56. monitoring of the photo degradation of amlodipine to it pyridine degradation product 26

58. HPLC-MS Studies

59. GC-MS Studies

60. TLC-MS Studies

61. CE-MS Studies

62. MEKC-MS and CEC-MS Studies

63. HPLC-NMR Studies27

65. HPLC-MS Studies

66. GC-MS Studies

67. TLC-MS Studies

68. CE-MS Studies

69. MEKC-MS and CEC-MS Studies

70. HPLC-NMR Studies28

74. auto-sampler

75. UV diode array detector

76. HP-MSD modelD mass spectrometer

77. thermo stated column selector

78. six-position Cheminert valve is inserted on “D” line of quaternary pump to extend mobile phase selection

79. Both column switcher and valve are connected through contact closures

81. 33 Modern approach COMET instrumentation fully automated Comprehensive Orthogonal Method Evaluation Technology (COMET)

82. 34 COMET instrumentation software

83. 35

84. 36

85. 37 Modern approach COMET instrumentation

87. highly selective

88. sensitive detection

89. wide ionisation capabilitiesAnise oil as starting material for the synthesis of 4-methoxy amphetamine was screened by GC-MS for impurities 38 Modern approach GC-MS

90. TLC-MS Separated spots on the plate could be subjected to direct matrix-assisted-laser-desorption ionization Time-of-flight mass spectrometry (TLC-MALDI TOF -MS) no need to remove the spots from plate Only wetting spot with methanol required to transfer the analyte from inside the silica gel to the surface thus enhancing the MALDI-TOF-MS signal 39 Modern approach TLC-MS MEOH TLC PLATE

91. 40 Modern approach Approaches for detection MS

92. majority of applications are from the fields of metabolite and natural product analyses stopped flow HPLC-NMR technique (together with HPLC-MS) in identifying impurities in acarbose 41 Modern approach LC-NMR

93. conclusion Impurity profiling is very important in the field of pharmaceutical analysis Unidentified and potentially toxic impurities are health hazards and in order to increase safety, impurity should be identified That’s all!!! 42

94. references Analysis of drug impurities Edited by Richard J. smith and michael L .Webb Blackwell publishing ICH guidelines Handbook of modern pharmaceutical analysis by satinder ahuja and stephan scypinski Volume III of SEPARATION SCIENCE AND TECHNOLOGY Recent Advances in the Impurity Profiling of Drugs Dorottya Bartos and Sándor Görög* Current Pharmaceutical Analysis, 2008, 4, 215-230 Characterization of a trace by‐product of the synthesis of the protease inhibitor tipranavir GE Martin, RH Robins, FW Crow… - Journal of …, 1999 - Wiley Online Library http://www.biolab.dk/sidevisning.asp?ID=674 www.wikipedia.org http://www.welsch.com/e/index.php5 http://www.thefullwiki.org/Gas_chromatography-mass_spectrometry Automated peak tracking for comprehensive impurity profiling in orthogonal liquid chromatographic separation using mass spectrometric detection Gang Xue∗, Anne D. Bendick Journal of Chromatography A, 1050 (2004) 159–171 43

95. 44

96. 45 HYDERABAD Thank you