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Prog Biomater ( impact factor-5.oo)
Presented by-
Vedant Kumar Gupta
Roll. No.- 9561011
M. Pharm 3rd Sem
Guide-
Dr. Ajay Kumar Yadav
Lecturer,
University Institute of
Pharmacy
C.S.J.M. University
Kanpur
Co-Guide-
Dr. N. P. Yadav
Principle Scientist
BPD Lab
CSIR-CIMAP
Lucknow
1
C. S. J. M. UNIVERSITY KANPUR
(UNIVERSITY INSTITUTE OF PHARMACY)
Contents
1. INTRODUCTION
2. METHODS OF BEADS FORMULATION
3. PREPARATION VARIABLES AND PROCESS OPTIMIZATION
4. EVALUATION PARAMETER
5. RESULTS AND DISCUSSION
6. CONCLUSION
7. REFERENCE
2
 To develop a multiparticulate system exploiting the pH-
sensitive property and biodegradability of calcium
alginate beads for intestinal delivery of Ceftriaxone
Sodium (CS) by oral route administration.
 To overcome the limitations of conventional immediate-
release, the oral drug delivery systems have been
developed, which provide sustained-release .
 The developed alginate beads formulation was able to
maintain steady plasma drug levels for extended periods
of time with reduced side effects
3
Purpose of this work
Introduction
 Beads are nearly spherical, solid and free flowing particulate carriers containing
dispersed drug particles either in solution or crystalline form.
 Beads size varies between 50µm-2mm
 Beads are produced from several polymers such as cationic polymers (e.g. chitosan),
anionic polymers (e.g. sodium alginate).
 Three different types of alginate beads, namely calcium alginate-chitosan beads,
calcium alginate-xanthan gum beads, and calcium alginate-maltodextrin beads.
 Alginate beads enteric coated with Cellulose acetate Phthalate (CAP), a pH-sensitive
polymer exhibited sustained release and deliver ceftriaxone sodium specifically to the
intestine.
4
 Sodium Alginate is a hydrophilic biopolymer and naturally occurring polysaccharide
obtained from brown seaweed and algae.
 Ceftriaxone belongs to a class of drugs called cephalosporin antibiotics used to
treat bacterial infections.
Advantages-
 Enhance drug stability
 Improve the bioavailability of acid labile drugs
 Reduced risk of local irritation
 Maintain steady plasma drug levels for extended periods of time
 Reduced side effects
5
 In this research paper authors followed the ionotropic gelation method.
 Total 12 batch of formulation developed.
 Calcium chloride was used as a crosslinking agent.
Methods
Ionotropic
gelation
Emulsion
gelation
Polyelectrolyte
complexation
6
Methods of beads formulation
Sodium alginate (0.4–1 % (w/v)) dissolved in deionized
water under magnetic stirring(1200- rpm) (2h)
add 2 mg of Ceftriaxone sodium dissolved in the Sodium
alginate solution and stirred ( 30 min)
Sonicated for 15 min
Drug-polymer solution introduced drop wise via a syringe
(22-guage) hypodermic needle into Calcium chloride
solution (0.2 to 4 % )
Cure (15 min)
Filtered (Whatman no. 42) and spread on petri dish, dried
(2 days) at room temperature and stored
Ionotropic gelation method
Fig. 1 Schematic diagram of the
preparation of beads by ionotropic
gelation method
7
 Beads were also prepared using polymers mixed with Sodium alginate such as Acacia,
Sodium carboxymethylcellulose, HPMC K4M and HPMC K15M .
Coating of beads
 Formulations F5, F6, F7 and F8 were selected for enteric coating with cellulose acetate
phthalate.
Beads dispersed in the coating solution (CAP 5 % w/v)
Stirred at 1200 rpm for 30 min at room temperature.
filtered
Spread on petri dish and dried for 2 days at room temperature
and stored
* Cellulose acetate Phthalate in 1:1 mixture of ethyl acetate and ethanol
8
Table -1
*Each formulation contains 2 mg of ceftriaxone sodium.
9
Preparation variables and process optimization
On the basis of the results obtained, the process parameters were optimized as follows:
 Sodium alginate concentration:- 1.25 % w/v,
 Sodium carboxymethylcellulose concentration:- 4.25 % w/v,
 Acacia concentration:- 2.5 % w/v,
 HPMC K4M concentration:- 1.875 % w/v,
 HPMC K15M concentration:- 1.25 % w/v,
 Calcium chloride concentration:- 3.75 % w/v,
 Curing time: 15 min, and curing speed: 60 rpm.
10
Evaluation parameter
1. Determination of percent yield, drug loading and entrapment efficiency
2. Thermal gravimetric analysis (TGA)
3. Swelling index study
4. Atomic force microscopy (AFM)
5. Determination of water content in alginate beads
6. Particle size analysis
7. In vitro drug release study
8. Analysis of release kinetics and mechanism
9. Loose surface crystal study (LSC)
10. Scanning electron microscopy (SEM)
11
Results and discussion
1. Determination of percent yield, drug loading and entrapment
efficiency-
 The entrapment efficiency of the uncoated formulation F5 possessing the highest
entrapment(67.8 ± 2.4 %) and F6 possessed lowest entrapment (38.2 ± 1.6 )
 The coated formulations F9 possessed the highest entrapment (74.7 ± 5.0 %),
whereas F10 had the lowest entrapment (40.9 ± 0.7 %)
 Drug loading range 0.07 ± 0.01 to 1.66 ± 1.39 % in all the formulations.
 Percent yield range of 24.9–93.6 %.
 F9 possessed the highest percent yield (93.6 %) and F1 possessed the lowest percent
yield (24.9 %).
12
Table 2 Effect of polymer concentration, Calcium chloride concentration, and coating
polymer concentration on percent yield and entrapment efficiency of various formulations.
13
2. Thermal gravimetric analysis (TGA)-
 Investigate the degradation and thermal stability of the beads. The thermograms (Fig. 3)
show a stepwise and sequential weight-loss pattern.
 Formulation F5 demonstrated smaller weight loss at high temperature ranges (4 %
between 420 and 550 ○C) during TGA.
 This indicates that beads formulated using sodium alginate and CMC had better thermal
stability than other formulations.
Fig. 3 Comparison of TGA thermograms of
pure alginic acid, pure CMC and
blank bead formulations of F1 to F8
14
3. Swelling index study-
 The swelling ratio of the beads depend on the pH of the solution in which the bead is
placed.
 The swelling behavior of the coated beads containing additional polymers (F9–F12) was
observed to be lower when compared to formulations F5–F8. This is because of the
presence of pH-sensitive enteric coating polymer covering the dense polymer matrix of
beads.
Swelling index = Wf – Wo/Wo
Table 3 Swelling index of calcium-alginate beads.
15
4. Atomic force microscopy (AFM)-
 Used to obtain information about the topographical features of the beads such as
morphology and roughness.
 The uncoated beads (Fig. 4a–d) have sharp, irregular and spiky projections on the surface,
indicating a coarse or rough texture.
 the coated beads (Figs. 4e–h) have smooth-edged projections, surfaces, and grooves.
Fig. 4 Topographic images of uncoated blank beads (upper row) of formulations a F5, b F6, c F7 and d F8; Topographic images
of coated blank beads (lower row) of formulations e F9, f F10, g F11, and h F12
16
5. Determination of alginate beads’ water content-
 The highest amount of water loss in formulation F8 may be attributed to the presence
of HPMC K15M due to the polymer’s ability to retain high amounts of water when
compared to other polymers.
 F6 demonstrated the least water loss, which is due to the rapid drying nature of acacia.
W1 % = [(Wo –Wd /Wo)] × 100
Table 4 Percent of water loss from calcium-alginate beads.
17
6. Particle size analysis-
 Used optical microscope
 Coated formulations (F9, F10, F11, and F12) have larger particle sizes compared to the
uncoated formulations (F5, F6, F7, and F8).
x =Ʃ(xi) / N
Table 5 Particle size of calcium-alginate beads.
18
7. In vitro drug release study-
 Within the first 2 h, 35–47 % of the drug was released in SGF from all the coated
formulations.
 The remaining part of the entrapped drug was released in the SIF, with sustained release
for up to 10 h in F10, 14 h in F11 and F12, and 18 h in F9
Fig. 6 In vitro drug release profile of ceftriaxone sodiumloaded formulations F9, F10, F11 and F12. Results indicate
mean % ±SD, (n = 3) 19
8. Analysis of release kinetics and mechanism-
 The kinetic models used to fit the in vitro release data were zero-order, first-order,
Higuchi, and Korsmeyer-Peppas models.
 The interpretation of data was based on the value of the correlation coefficients.
 it can be concluded that the release kinetics for all the coated formulations (F9–F12) can
be best described by the first-order model.
Table 6 In vitro release kinetic parameters of ceftriaxone sodium beads coated with cellulose acetate
phthalate
20
9. Loose surface crystal (LSC)-
 Determine the amount of the drug present on or near the surface of the beads.
 LSC was highest in the F10 formulation, whereas it was lowest in formulation F11.
Table 7 Percentage of loose surface crystals of ceftriaxone sodium on calcium-alginate beads.
21
10. Scanning electron microscopy (SEM)-
 Based on the entrapment efficiency and in vitro results, formulations F5 and F9 were
chosen for the SEM studies.
 SEM micrographs of the blank formulation (Fig. 7a–b) show that the beads were almost
spherical, with a rough outer surface.
 From the images (Fig. 7c–d), F5 beads can be seen to possess a rough surface with a
large number of pores that cause the rapid release of drug into the in vitro release
medium.
 SEM images (Fig. 7e–f) of coated beads (F9) show a smooth surface and possibly a
reduced number of pores due to the presence of the coating, which lead to a decrease in
the drug release rate from beads.
Fig. 7 SEM images—blank formulation F5 at a low
magnification, and b at high magnification; c drug-
loaded formulation F5 low magnification, and d high
magnification; e drug-loaded CAP-coated
formulation F9 at low magnification, and f high
magnification
22
Conclusion
 Sodium CMC, HPMC K4M, HPMC K15M and acacia as drug release modifiers.
 Optimized parameters achieved high entrapment efficiency, proper particle size,
swelling behavior, and surface morphology.
 use of sodium alginate, carboxymethylcellulose and cellulose acetate phthalate
decreased the drug release behavior in gastric conditions
 Give sustained drug release at intestinal pH.
 The drug entrapment efficiency of the optimized formulation was 75 ± 5 %.
 Swelling properties of drug loaded beads were found to be in a range of 0.9–3.4.
 The particle size of the beads was between 1.04 ± 0.20 and 2.15 ± 0.36 mm.
23
Reference
 Patel N, Lalwani D, Gollmer S, Injeti E, Sari Y, Nesamony J. Development and
evaluation of a calcium alginate based oral ceftriaxone sodium formulation. Progress
in biomaterials. 2016 Jul;5(2):117-33.
24
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Developing pH-Sensitive Calcium Alginate Beads for Intestinal Delivery of Ceftriaxone Sodium

  • 1. Prog Biomater ( impact factor-5.oo) Presented by- Vedant Kumar Gupta Roll. No.- 9561011 M. Pharm 3rd Sem Guide- Dr. Ajay Kumar Yadav Lecturer, University Institute of Pharmacy C.S.J.M. University Kanpur Co-Guide- Dr. N. P. Yadav Principle Scientist BPD Lab CSIR-CIMAP Lucknow 1 C. S. J. M. UNIVERSITY KANPUR (UNIVERSITY INSTITUTE OF PHARMACY)
  • 2. Contents 1. INTRODUCTION 2. METHODS OF BEADS FORMULATION 3. PREPARATION VARIABLES AND PROCESS OPTIMIZATION 4. EVALUATION PARAMETER 5. RESULTS AND DISCUSSION 6. CONCLUSION 7. REFERENCE 2
  • 3.  To develop a multiparticulate system exploiting the pH- sensitive property and biodegradability of calcium alginate beads for intestinal delivery of Ceftriaxone Sodium (CS) by oral route administration.  To overcome the limitations of conventional immediate- release, the oral drug delivery systems have been developed, which provide sustained-release .  The developed alginate beads formulation was able to maintain steady plasma drug levels for extended periods of time with reduced side effects 3 Purpose of this work
  • 4. Introduction  Beads are nearly spherical, solid and free flowing particulate carriers containing dispersed drug particles either in solution or crystalline form.  Beads size varies between 50µm-2mm  Beads are produced from several polymers such as cationic polymers (e.g. chitosan), anionic polymers (e.g. sodium alginate).  Three different types of alginate beads, namely calcium alginate-chitosan beads, calcium alginate-xanthan gum beads, and calcium alginate-maltodextrin beads.  Alginate beads enteric coated with Cellulose acetate Phthalate (CAP), a pH-sensitive polymer exhibited sustained release and deliver ceftriaxone sodium specifically to the intestine. 4
  • 5.  Sodium Alginate is a hydrophilic biopolymer and naturally occurring polysaccharide obtained from brown seaweed and algae.  Ceftriaxone belongs to a class of drugs called cephalosporin antibiotics used to treat bacterial infections. Advantages-  Enhance drug stability  Improve the bioavailability of acid labile drugs  Reduced risk of local irritation  Maintain steady plasma drug levels for extended periods of time  Reduced side effects 5
  • 6.  In this research paper authors followed the ionotropic gelation method.  Total 12 batch of formulation developed.  Calcium chloride was used as a crosslinking agent. Methods Ionotropic gelation Emulsion gelation Polyelectrolyte complexation 6 Methods of beads formulation
  • 7. Sodium alginate (0.4–1 % (w/v)) dissolved in deionized water under magnetic stirring(1200- rpm) (2h) add 2 mg of Ceftriaxone sodium dissolved in the Sodium alginate solution and stirred ( 30 min) Sonicated for 15 min Drug-polymer solution introduced drop wise via a syringe (22-guage) hypodermic needle into Calcium chloride solution (0.2 to 4 % ) Cure (15 min) Filtered (Whatman no. 42) and spread on petri dish, dried (2 days) at room temperature and stored Ionotropic gelation method Fig. 1 Schematic diagram of the preparation of beads by ionotropic gelation method 7
  • 8.  Beads were also prepared using polymers mixed with Sodium alginate such as Acacia, Sodium carboxymethylcellulose, HPMC K4M and HPMC K15M . Coating of beads  Formulations F5, F6, F7 and F8 were selected for enteric coating with cellulose acetate phthalate. Beads dispersed in the coating solution (CAP 5 % w/v) Stirred at 1200 rpm for 30 min at room temperature. filtered Spread on petri dish and dried for 2 days at room temperature and stored * Cellulose acetate Phthalate in 1:1 mixture of ethyl acetate and ethanol 8
  • 9. Table -1 *Each formulation contains 2 mg of ceftriaxone sodium. 9
  • 10. Preparation variables and process optimization On the basis of the results obtained, the process parameters were optimized as follows:  Sodium alginate concentration:- 1.25 % w/v,  Sodium carboxymethylcellulose concentration:- 4.25 % w/v,  Acacia concentration:- 2.5 % w/v,  HPMC K4M concentration:- 1.875 % w/v,  HPMC K15M concentration:- 1.25 % w/v,  Calcium chloride concentration:- 3.75 % w/v,  Curing time: 15 min, and curing speed: 60 rpm. 10
  • 11. Evaluation parameter 1. Determination of percent yield, drug loading and entrapment efficiency 2. Thermal gravimetric analysis (TGA) 3. Swelling index study 4. Atomic force microscopy (AFM) 5. Determination of water content in alginate beads 6. Particle size analysis 7. In vitro drug release study 8. Analysis of release kinetics and mechanism 9. Loose surface crystal study (LSC) 10. Scanning electron microscopy (SEM) 11
  • 12. Results and discussion 1. Determination of percent yield, drug loading and entrapment efficiency-  The entrapment efficiency of the uncoated formulation F5 possessing the highest entrapment(67.8 ± 2.4 %) and F6 possessed lowest entrapment (38.2 ± 1.6 )  The coated formulations F9 possessed the highest entrapment (74.7 ± 5.0 %), whereas F10 had the lowest entrapment (40.9 ± 0.7 %)  Drug loading range 0.07 ± 0.01 to 1.66 ± 1.39 % in all the formulations.  Percent yield range of 24.9–93.6 %.  F9 possessed the highest percent yield (93.6 %) and F1 possessed the lowest percent yield (24.9 %). 12
  • 13. Table 2 Effect of polymer concentration, Calcium chloride concentration, and coating polymer concentration on percent yield and entrapment efficiency of various formulations. 13
  • 14. 2. Thermal gravimetric analysis (TGA)-  Investigate the degradation and thermal stability of the beads. The thermograms (Fig. 3) show a stepwise and sequential weight-loss pattern.  Formulation F5 demonstrated smaller weight loss at high temperature ranges (4 % between 420 and 550 ○C) during TGA.  This indicates that beads formulated using sodium alginate and CMC had better thermal stability than other formulations. Fig. 3 Comparison of TGA thermograms of pure alginic acid, pure CMC and blank bead formulations of F1 to F8 14
  • 15. 3. Swelling index study-  The swelling ratio of the beads depend on the pH of the solution in which the bead is placed.  The swelling behavior of the coated beads containing additional polymers (F9–F12) was observed to be lower when compared to formulations F5–F8. This is because of the presence of pH-sensitive enteric coating polymer covering the dense polymer matrix of beads. Swelling index = Wf – Wo/Wo Table 3 Swelling index of calcium-alginate beads. 15
  • 16. 4. Atomic force microscopy (AFM)-  Used to obtain information about the topographical features of the beads such as morphology and roughness.  The uncoated beads (Fig. 4a–d) have sharp, irregular and spiky projections on the surface, indicating a coarse or rough texture.  the coated beads (Figs. 4e–h) have smooth-edged projections, surfaces, and grooves. Fig. 4 Topographic images of uncoated blank beads (upper row) of formulations a F5, b F6, c F7 and d F8; Topographic images of coated blank beads (lower row) of formulations e F9, f F10, g F11, and h F12 16
  • 17. 5. Determination of alginate beads’ water content-  The highest amount of water loss in formulation F8 may be attributed to the presence of HPMC K15M due to the polymer’s ability to retain high amounts of water when compared to other polymers.  F6 demonstrated the least water loss, which is due to the rapid drying nature of acacia. W1 % = [(Wo –Wd /Wo)] × 100 Table 4 Percent of water loss from calcium-alginate beads. 17
  • 18. 6. Particle size analysis-  Used optical microscope  Coated formulations (F9, F10, F11, and F12) have larger particle sizes compared to the uncoated formulations (F5, F6, F7, and F8). x =Ʃ(xi) / N Table 5 Particle size of calcium-alginate beads. 18
  • 19. 7. In vitro drug release study-  Within the first 2 h, 35–47 % of the drug was released in SGF from all the coated formulations.  The remaining part of the entrapped drug was released in the SIF, with sustained release for up to 10 h in F10, 14 h in F11 and F12, and 18 h in F9 Fig. 6 In vitro drug release profile of ceftriaxone sodiumloaded formulations F9, F10, F11 and F12. Results indicate mean % ±SD, (n = 3) 19
  • 20. 8. Analysis of release kinetics and mechanism-  The kinetic models used to fit the in vitro release data were zero-order, first-order, Higuchi, and Korsmeyer-Peppas models.  The interpretation of data was based on the value of the correlation coefficients.  it can be concluded that the release kinetics for all the coated formulations (F9–F12) can be best described by the first-order model. Table 6 In vitro release kinetic parameters of ceftriaxone sodium beads coated with cellulose acetate phthalate 20
  • 21. 9. Loose surface crystal (LSC)-  Determine the amount of the drug present on or near the surface of the beads.  LSC was highest in the F10 formulation, whereas it was lowest in formulation F11. Table 7 Percentage of loose surface crystals of ceftriaxone sodium on calcium-alginate beads. 21
  • 22. 10. Scanning electron microscopy (SEM)-  Based on the entrapment efficiency and in vitro results, formulations F5 and F9 were chosen for the SEM studies.  SEM micrographs of the blank formulation (Fig. 7a–b) show that the beads were almost spherical, with a rough outer surface.  From the images (Fig. 7c–d), F5 beads can be seen to possess a rough surface with a large number of pores that cause the rapid release of drug into the in vitro release medium.  SEM images (Fig. 7e–f) of coated beads (F9) show a smooth surface and possibly a reduced number of pores due to the presence of the coating, which lead to a decrease in the drug release rate from beads. Fig. 7 SEM images—blank formulation F5 at a low magnification, and b at high magnification; c drug- loaded formulation F5 low magnification, and d high magnification; e drug-loaded CAP-coated formulation F9 at low magnification, and f high magnification 22
  • 23. Conclusion  Sodium CMC, HPMC K4M, HPMC K15M and acacia as drug release modifiers.  Optimized parameters achieved high entrapment efficiency, proper particle size, swelling behavior, and surface morphology.  use of sodium alginate, carboxymethylcellulose and cellulose acetate phthalate decreased the drug release behavior in gastric conditions  Give sustained drug release at intestinal pH.  The drug entrapment efficiency of the optimized formulation was 75 ± 5 %.  Swelling properties of drug loaded beads were found to be in a range of 0.9–3.4.  The particle size of the beads was between 1.04 ± 0.20 and 2.15 ± 0.36 mm. 23
  • 24. Reference  Patel N, Lalwani D, Gollmer S, Injeti E, Sari Y, Nesamony J. Development and evaluation of a calcium alginate based oral ceftriaxone sodium formulation. Progress in biomaterials. 2016 Jul;5(2):117-33. 24
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