Choices and Trends in Solid Dosage Form Selection

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Lecture 1: Preformulation and Biopharmaceutical Considerations in Drug Product Design and Development

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Lecture 6: Biopharmaceutic Considerations

Lecture 2: Drug Substance Physical Form Selection

Lecture 7: Chemical Stability Assessment in Preformulation

Lecture 3: Drug Substance Physical Form Characterization

Lecture 8: Excipient Compatibility Studies

Lecture 4: Solubility: General Principles and Practical Considerations

Lecture 9: Impact of Material Properties on Formulation Development

Lecture 5: Dissolution and its Role in Solid Oral Dosage Form Development

Lecture 10: Prototype Formulations Screening and Characterization

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Join us September 24, 2015 for the 9th Session!

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“2015 Drug Design and Delivery Symposium: Choices and Trends in Solid Dosage Form Selection”

Rao Mantri Bristol-Myers Squibb

Scott Trzaska J-Star Research

Ronald Smith Merck

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The 2015 Drug Design and Delivery Symposium is co-produced by the ACS Medicinal Chemistry Division and the AAPS

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Choices and Trends in Solid Dosage Form Selection: Salt, Cocrystal, Prodrug or Amorphous?

Scott Trzaska, J-Star Research

Ron Smith, Merck

August 27, 2015

Pharmaceutical Materials Particle Attributes O

API

OH

Solid State Form

O

O

Drug Product

Formulated Intermediate 16

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Form, Attributes, and Formulation

Solid State Form

Formulation

Stability Robust Crystallization Solubility

Enteric Coating Dispersions Solutions

Particle Attributes Filtration rates Content Uniformity Dissolution rate

Bioperformance

Manufacturability

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Solid State Forms • Polymorphs • Hydrates and solvates • Salts

+

• Cocrystals • Amorphous ++

++

-

-

-

-

-

+ + + +

-

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Prodrug

“Prodrugs in Drug Discovery” Thursday, November 19, 2015

John Higgins, Senior Principal Scientist, Discovery Pharmaceutical Sciences at Merck 19

The Ideal Solid State Form • Good biological performance • Suitable solid-state properties • Acceptable chemical and physical stability

• Manufacturing ease • Minimal risk 20

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Considerations • Phase of the program

• Indication • Dose • Formulation • Long term strategy 21

Solid State Form Selection Screen for crystalline candidates

Identify thermodynamic relationships Biological, physical, chemical, and mechanical properties Scale up Selection 22

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Identify thermodynamic relationships Biological, physical, chemical, and mechanical properties Scale up

Selection 23

Screening Tools

Vapor Diffusion

Melt Crystallizations

Automated Crystallizations

Isothermal Crystallizations Sonication Induced Nucleation Variable Temperature Solvent Drop Grinding

Controlled Heating and Cooling

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Screening Techniques • Solution temperature cycling

• Slurry conversions

• Evaporative crystallizations

• Solid state temperature cycling

• Solvent vapor diffusion into solids • Antisolvent addition to solutions • Laser induced crystallization

• Mechanical activation

• Sublimation

• pH swings

Newman, A. Organic Process Research and Development 2013, 17 (3), 457 - 471, Specialized Solid Form Screening Techniques Lee, E. H. Asian Journal of Pharmaceutical Sciences 2014, 9 (4), 163 - 175, A Practical Guide to Pharmaceutical Polymorph Screening & Selection

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Identify thermodynamic relationships Biological, physical, chemical, and mechanical properties Scale up Selection 26

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Thermodynamic Relationships • Temperature, pressure, and water activity • Polymorphs o Most stable o Transition temperatures

• Solvates and hydrates o Temperatures o Activities

• Salts • Cocrystals • Amorphous systems 27

Thermodynamics: Polymorphs • Monotropic • Enantiotropic • Transition temperature • Techniques oSolubility oSlurry transformations oCalorimetry

Miller, M. J.; Collman, B. M.; Greene, L. R.; Grant, D. J. W.; Blackburn, A. C. Pharmaceutical Development and Technology 2005, 10, 291 – 297, Identifying the Stable Polymorph Early in the Drug Discovery – Development Process Yu, L. Journal of Pharmaceutical Sciences 1995, 84, 966 – 974, Inferring Thermodynamic Stability Relationship of Polymorphs from Melting Data

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Most Stable Form: Solubility Form 3 Form 1

Form 2

Solubility

DG Form 1 Form 2 = RT ln (X2 /X1) DG Form 2 Form 3 = RT ln (X3 /X2) Ttransition

T

Form 2 is always more stable than Form 1, monotropic

Form 3 is more stable than Form 2 below Ttransition, enantiotropic

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Most Stable Form: Slurries • Diverse solvent systems o Functional groups, polarity, hydrogen bonding, activity

• Vary temperature • Days to weeks Form 1 [10 mg/mL]

Form 2 [5 mg/mL]

Solution

Form 1

Form 1

Form 1+2

Solvate

Form 2

Form 2

Gu, C.; Li, H.; Gandhi, R. B.; Raghavan, K. International Journal of Pharmaceutics 2004, 283, 117 – 125, Grouping Solvents by Statistical Analysis of Solvent Property Parameters: Implications to Polymorph Screening

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Thermodynamics: Hydrates • Understand relationship of anhydrous form and hydrate • Temperature • Pressure

• Water activity

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Anhydrous Versus Hydrate • Chemical potential impacts relative stability • mw = mw° + RT ln aw aw = gwXw mw = mw° + RT ln (gwXw) • Hydrate favored at high mw – T

–  aw (Xw)

• Anhydrous form favored at low mw – T –  aw (Xw)

• Anhydrous form is stable above critical T and below critical aw

+ 32

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Literature Example: Amgen • Originally isolating an anhydrous form • A hemihydrate was discovered during development

aw > 0.452, 25 °C

Anhydrous

Hemihydrate aw < 0.452, 25 °C

Morrison, H.; Quan, B. P.; Walker, S. D.; Hansen, K. B.; Nagapudi, K.; Cui, S. Organic Process Research and Development ASAP Article, DOI: 10.1021/acs.oprd.5b00030, Appearance of a New Hydrated Form during Development: A Case Study in Process and Solid-State Optimization

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Thermodynamics: Salts • Disproportionation • pH max • Excipients

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Solid-Solution Equilibria

B = Weak Base Ka

BH+Cl- = High Solubility

Solubility (mg/mL)

0

2

B + H+ + Cl-

Ssalt

S0

BH+Cl- (s)

4

S0 pHmax  pKa  log Ssalt

6

B = Low Solubility

BH+ + Cl-

B (s) 8

pH

10

12

14

pHmax

Serajuddin, A. T. M. Advanced Drug Delivery Reviews 2007, 59, 603 - 616, Salt Formation to Improve Drug Solubility

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Thermodynamics: Cocrystals • Ternary Phase diagram Solvent

API Cocrystal

Cocrystal Former 36

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Thermodynamics: Cocrystals • Ternary Phase diagram Solvent

API Cocrystal

Cocrystal Former 37

Thermodynamics: Amorphous • Dispersion – phase separation • Crystallization risk

• Humidity

Meng, F.; Dave, V.; Chauhan, H. European Journal of Pharmaceutical Sciences 2015, 77, 106 - 111, Qualitative and Quantitative Methods to Determine Miscibility in Amorphous Drug-Polymer Systems

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Selection 39

Properties Biological Performance • Solubility • Dissolution Rate • Particle Attributes • Excipients

Physical Stability • Thermodynamic stability • Risk of a form change • Processing space

Chemical Stability • Oxidation • Hydrolysis • Photochemical • Thermal decomposition

Mechanical Stability • Physical impact • Pressure • Disorder 40

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Selection 41

Scale Up • Thermodynamic or kinetic control? • Can the form be manufactured? o o o o

Crystallization Filtration Solvent removal Particle attribute control

• Can the form be formulated? 42

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Selection 43

Salts of Weak Acids and Bases: In Vivo Behavior Salts of acid 1-3

pH

4.5-6.8

• Can precipitate in the stomach in an uncontrolled fashion • May “parachute” in solution (supersaturation) • Free acid solubility increases with transit

Salts of base •

•

Stomach conditions favor the acid addition salts of bases Rate and extent of absorption depends on: o Dissolution in stomach o Precipitation vs absorption kinetics o Absorption window (site of absorption) 44

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Case Example: Ifetroban Sodium O- Na+

O O- Na +

O O N O O

O

O N

N N

O

• • • • •

Weak acid (pKa = 4.5) Solubility of sodium salt > 700 mg/mL Solubility of free acid = 0.007 mg/mL Conversion of Na salt to free acid in dosage form (micro-environmental pH) High solubility ration (salt to free form) not always desired

Serajuddin et. al., J. Pharm. Sci., 88(7), 696-704, 1999

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Case Example: Atazanavir Sulfate

4

Solubility (mg/mL)

3

S a l t

F r e e B a s e

2 p H a d j u s t e d w i t h H C l p H a d j u s t e d w i t h H 2 S O 4

• • •

1

• 0

0 1 2 3 4 5 6 7 8

•

p H

• US Patent: 6,087,383

Weak base (pKa = 4.7) Solubility

Choices and Trends in Solid Dosage Form Selection

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