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Home J Young Pharm. Vol 15/Issue 4/2023 A Comprehensive Overview of Edible Natural Excipients and their Potential Use in Pharmaceutical Formulation Development
J Young Pharm. Vol 15/Issue 4/2023

A Comprehensive Overview of Edible Natural Excipients and their Potential Use in Pharmaceutical Formulation Development

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Jahnabi Sarmah1, Ananta Choudhury1*, Himangshu Deka1, Debgopal Ganguly2, Dhiraj Baishya1 and Rosamund Jyrwa3
Author informationArticle notesCopyright and License informationPDFCitations

1Faculty of Pharmaceutical Science, Assam Down Town University, Panikhaiti, Guwahati, Assam, INDIA

2NSMS Institute of Pharmacy, Nachan Road, Kamalpur, Durgapur, Paschim Bardhaman, West Bengal, INDIA

3Pratiksha Institute of Pharmaceutical Sciences, Chandrapur Rd, Near Central Training Center, Panikhaiti, Barchapari, Assam, INDIA

Corresponding author.

Correspondence: Dr. Ananta Choudhury, Faculty of Pharmaceutical Science, Assam Down Town University, Sankar Madhab Path Gandhi Nagar, Panikhaiti, Guwahati-781026, Assam, INDIA, Email: [email protected], ORCID: 0000-0002-6894-1670
Received May 22, 2023; Revised July 01, 2023; Accepted July 22, 2023.
Copyright ©2023 Author (s)
This is an open access article distributed under the terms of the Creative Commons Attribution-NonCommercial-ShareAlike 4.0 License, which allows others to remix, tweak, and build upon the work non-commercially, as long as the author is credited and the new creations are licensed under the identical terms.

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1.Ganguly D, Choudhury A, Chanda R, Das H, Mitra S, Ghosh R, et al. Nanoparticulate Formulation for the Treatment of Different Types of Colon Disease Like Ulcerative Colitis: A Comprehensive Review. Journal of Young Pharmacists [Internet]. 2023 Dec 22;15(4):585–8. Available from: http://dx.doi.org/10.5530/jyp.2023.15.82
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Published in: Journal of Young Pharmacists, 07 December 2023; 15(4): 589-594.Published online: 07 December 2023DOI: 10.5530/jyp.2023.15.83

ABSTRACT

This review aims to explore the prospective scope of excipients obtained from edible natural sources and its unique application in the field of pharmaceutical formulation development. A systematic literature search was conducted using data base like PubMed, Science Direct, Embase, and Google Scholar. A total of 50 articles were identified and reviewed, which primarily focused on the unique application of edible natural sources as excipients in the field of pharmaceutical formulation development. The results revealed that edible natural sources like Dillenia indica, Abelmoschus esculentus; Oryza sativa L; Artocarpus heterophyllus; Tamarindus indica; Musa paradisiaca; Mangifera indica; Ipomoea batatas; Hibiscus sabdariffa and Solanum tuberosum are a promising source of excipients and have great potential to be used in the formulation of pharmaceutical dosage form. Furthermore, the use of these sources may potentially reduce the costs associated with the production of pharmaceuticals dosage form and could also improve the safety profile of the drugs. The review highlights the importance of the use of edible natural sources as excipients and their potential to revolutionize the field of pharmaceutical formulation development.

Keywords: Edible natural substance, Excipients, Diluents, Natural binders, Pharmaceutical formulation

INTRODUCTION

The pharmaceutical formulation development industry is increasingly making use of excipients derived from edible natural sources, as they have been proven to effectively stabilize, boost solubility, absorption, and bioavailability of Active Pharmaceutical Ingredients (APIs). Some natural excipients that have been explored as an alternative to synthetic ones are starches, celluloses, gums, and pectins.1 These natural excipients have the potential to improve the properties of formulations, reduce manufacturing costs, and increase patient compliance.2 Some of the potential applications of edible natural excipients in pharmaceutical formulation development include use of Natural excipients such as Hydroxypropyl Methylcellulose (HPMC) and Polyethylene Glycol (PEG) can be used to solubilize poorly soluble APIs.3 Natural excipients such as gum arabic, xanthan gum, and carrageenan can be used to stabilize and suspend poorly soluble APIs in aqueous media. Further, natural excipients like pectin and carrageenan can be used to form micro- and nano-encapsulated particles of APIs.4 Again natural excipients such as starches, celluloses, and gums are used as binders, fillers, and disintegrants in formulation of tablet dosage form. Similarly, gum arabic can be used to form enteric and resistance coatings on tablets.5 These are just a few examples of the potential applications of edible natural excipients in pharmaceutical formulation development. With the increasing demand for natural, safe, and effective formulations, there is a great opportunity for further exploration of edible natural excipients in pharmaceutical formulation development.6 Considering the above fact this article has been prepared to explore the prospective scope of excipients obtained from edible natural sources and their unique application in the field of pharmaceutical formulation development

METHODOLOGY

The search strategy for this systematic review was designed to identify relevant studies on the prospective scope of excipients obtained from edible natural sources and its unique application in the field of pharmaceutical formulation development. The search was conducted using the following databases: PubMed, ScienceDirect, Wiley Online Library, and Google Scholar. The following keywords were used: “excipient”, “natural source”, “edible”, “formulation”, “development”, and “pharmaceutical”. The search was limited to articles published in the English language from 2010 to 2022. Studies were included if they addressed the prospective scope of excipients obtained from edible natural sources and its application in the field of pharmaceutical formulation development. The reported literature provides conclusive information about the various natural sources that serve as effective excipients Figure 1. Hence, the outputs of the present study are expected to lead towards the findings of effective excipients.

DISCUSSION

The information about some edible natural resources that play a significant role as excipient in the field of formulation design and development are as follows (Table 1).

Abelmoschus esculentus

The plant Abelmoschus esculentus belongs to the family of Malvaceae. It is popularly known as lady’s-fingers, okra and bhindi in India and Southeast Asia. It is a tropical to subtropical plant that is generally appropriated across Africa to Asia, Southern Europe, and America. Apart from its use as edible vegetables, the polysaccharides obtained from the fruit part play certain clinical role in design of modern dosage form.7 The research conducted on okra has revealed that its mucilage, which is retrieved from the seed and fruit part, is a great source of pectin. This mucilage showed considerable suspending properties when tested in Acetaminophen pediatric suspension at low concentrations.8 Moreover, okra powder was discovered to possess disintegrating properties when used in small amounts.9 Recently, there has been an increasing focus on the role of okra mucilage as a binder in tablet formulations. It has also been suggested as an alternative excipient for the development of sustained-release tablet formulations.10 Additionally, the gum from okra has been explored for gastric floating dosage forms, yet it has been reported to have limited buoyancy. 11

Artocarpus heterophyllus

Artocarpus heterophyllus belongs to the family of Moraceae and commonly known as jackfruit or Ceylon jack. It contains tacky or sticky white latex. Veggie lovers and vegans regularly utilize this organic product as a substitute of meat. It is reported that Jackfruit seeds is a good source of starch.12 The powder of Artocarpus heterophyllus seeds has been found to be an effective binder in the formulation of paracetamol tablets.13 In comparison to commercial starch, the binding ability of jackfruit seed starch is significantly superior.14 A recent study has developed Cross-Linked Carboxymethyl Jackfruit Starch (CL-CMJF) and used it effectively as a tablet disintegrant.15 Additionally, jackfruit seed starch powder was employed as a super disintegrant in the formulation of fast dissolving tablets.16 Further, Jackfruit latex has been identified as a potential natural binder that can be used to construct mucoadhesive solid dosage forms and oral sustained-release tablets.17 The mucilage obtained from the ripe fruit pulp of A. heterophyllus has multifunctional properties, which could be beneficial in various applications.

Figure 1:
Literature selection process for the study.

Colocasia esculenta

Colocasia esculenta, a yearly herbaceous plant of the family Araceae, has been utilized in traditional medicine in many nations for centuries. This tropical plant is primarily grown for its edible corms, which are also known as taro and are used as a vegetable in numerous cuisines all over the world. A recent study compared the use of Colocasia esculenta starches with that of maize starch and found it to be a viable substitute for binder and disintegrant in tablet production due to its high starch content.18 Taro (Colocasia esculenta) starch has been found to be a more efficient disintegrant than potato or maize starch. In order to modify its structure, pregelatinizing is done. This modified form of Taro starch has been successfully used as diluents in the production of Thiamine Hydrochloride tablets.19 Matrix tablets with antiviral properties for sustained release were designed using Taro gum, a natural polymer derived from Taro corms (Taro root). This gum has been explored for its mucoadhesive strength and its capacity to slow the rate of release of the drug.20 As such, it has been found to be a suitable excipient for the design of controlled drug delivery.21

Hibiscus sabdariffa

Hibiscus sabdariffa, commonly known as roselle or Tenga mora, is a restorative plant that is widely distributed in tropical and subtropical areas across the world. It is capable of adapting to a variety of soils in hot and humid environments. Roselle is popular for its high source of beta-carotene, vitamin C, protein, and total sugar, as well as its nutritional and medicinal properties. Different parts of the plant, such as seeds, leaves, fruits, and roots, are used in various foods as herbal supplements and are believed to treat various medical conditions, including various cardiovascular problems, helminthic diseases, and cancer.22 Hibiscus sabdariffa has traditionally been used as a food, herbal drink, seasoning or flavouring agent in the food industry, and as a natural or herbal medication. In a recent study, the efficacy of the mucilage obtained from the fresh leaves of H. sabdariffa as a binder was evaluated in an Orodispersible tablet.23 The mucilage from the Hibiscus sabdariffa leaves was compared with other binding agents such as starch and Poly Vinyl Pyrrolidine (PVP) and was found to have a higher binding capacity than starch and PVP. Additionally, in another study, H. sabdariffa calyx extract was used as a colouring agent in a pharmaceutical formulation.24 In a further study of the development and evaluation of Fast Dissolving Tablets, the effective disintegration properties of H. sabdariffa mucilage were evaluated and found to be satisfactory.25

Ipomoea batatas

Ipomoea batatas are commonly known as sweet potatoes belong to the family Convolvulaceae. It is dicotyledonous plants that are utilized as a root vegetable. They are a decent or good source of fiber, potassium, vitamins, and other fundamental nutrients.26 Sweet potato starch could be obtained from the root of Ipomoea batatas. Sweet potato roots contain around 70% starch. It is used as a binder, disintegrant, and diluents. The modified sweet potato starch has better pharmaceutical properties than native starch. Starch from local sweet potato needs a chemical modification process to produce derivatives with better specific pharmaceutical characteristics for the production of tablets. Sweet potato starch was used as a binder in the development of lozenge dosage form.27 As per the literature, sweet potato starch shows its efficiency as disintegrant as well as binding agent in preparation of different tablet formulation. A comparative study states that sweet potato starch has better binding capacity compared to maize starch. Further, A study by Jubril et. al., reflect that due to the high hydration and swelling capacities the modified sweet potato starch shows stronger disintegrant property than the unmodified sweet potato starch.28 The high-density nature of sweet potato starch makes it choice suitable as diluents.29,30

Mangifera indica

Mangifera indica most commonly known as mango tree belongs to the family Anacardiaceae, is a huge evergreen tree. Mango the fruit of the tree is the most tropical organic product that are originated from the region between northwestern Myanmar, Bangladesh, and India31 Mango fruits are reported to have a high nutritional value and pharmacological properties like antioxidant, immunomodulation, cardio tonic, hypotensive, wound healing, anti-degenerative, and antidiabetic activities.32 The mature seeds of Mangifera indica is a as rich sources of starch. The starch obtained from seeds of M. indica was used as an excipient (binder and disintegrating agent) in the formulation of Paracetamol and Ibuprofen tablet.33 Further, the Mangifera indica peel contains a good percentage of pectin.34 Fast dissolving tablets of furosemide were formulated by direct compression method using pectin derived from mango peel as natural disintegrants, the result of the study states that pectin powder of M. indica shows better drug release and disintegration time as compared to tablets prepared from other natural and synthetic disintegrants.35 The Mango (Mangifera indica) gums were successfully used in the design of matrix tablets of Glibenclamide and sustained-release tablets of Diclofenac sodium at a lower concentration.36

Musa paradisiaca

Musa paradisiaca is popularly known as a banana belongs to the family, Musaceae. More than 700 varieties, 30 notable species within the genus Musa are available. It is a popular fruit with high nutritional value and a wide range of health benefits.37 Banana starch has been obtained from the unripe fruit of the plant Musa paradisiaca. The binding properties of Musa paradisiaca were investigated, evaluated, and found that it could be used as a binding agent in the formulation of solid dosage form.38 A comparative binding study of banana starch with maize BP and Polyvinyl Pyrrolidone (PVP) reflect the advantages of banana starch as an effective binder.39 Further, a comparative study of banana starch with potato starch and corn starch for the disintegrant properties reflect superiority of the banana starch powder as disintregant in a fast disintegrating tablet.40 Further, pectin obtained from banana peels were successfully used as pharmaceutical excipient to prepare solid as well as the semisolid dosage form. The waste peel of the banana was processed and employed as adhesive in paracetamol tablets. Moreover, mucoadhesive property of Crude banana powder was also found to be effective.41

Oryza sativa

Oryza sativa, usually known as Asian rice, is the plant species most commonly referred as English rice. Further, “Bora Chaval” is a nutritious grain crop mostly consumed by people of North-east India having high amylopectin content. The Bora rice is the rich source of pregelatinized starch (90%) that is used in directly compressible tablet as excipient.42,43 It is also reported that the level of crystallinity of Assam Bora rice starch is significantly higher than potato starch, which mirrors its obstruction towards enzymatic hydrolysis during digestion in the gastrointestinal tract. It shows better binding property as compared to gelatin powder.44,45 Further, in an evaluation of several native starches, rice starch proved to have much better compaction properties than potato, maize, and tapioca starch. The starch of Oryza sativa L. was reported to use as a biopolymer. Further, it was successfully used as natural mucoadhesive matrix agent for the formulation of controlled release drug delivery. Assam Bora rice starches also possess good disintegrating properties.

Sl.No. Botanical Name Family Local name Parts used Excipient use References
1 Abelmoschus esculentus Linn. Malvaceae Bhindi, Okra Fruit Binder, Disintegrant, Suspending agent, Polymer. 8-11
2 Artocarpus heterophyllus Moraceae Jackfruit Seed starch, Mucilage, Fruit latex Binder, Disintegrant, Super disintegrant, Polymer. 14-17
3 Solanum tuberosum Solanaceae Potato Starch tuber Binder, Diluent, Disintegrant. 47
4 Colocasia esculenta Araceae Taro Taro gum, Starch Binder, Disintegrant, Diluent, Polymer. 18-21
5 Hibiscus sabdariffa Malvaceae Roselle, Tenga mora Mucilage from leaves and fruit catalyce Binder, Disintegrant, Colouring agent. 22,24,26
6 Ipomoea batatas Convolvulaceae Sweet Potato Starch Binder and Diluent, Disintegrant, Polymer. 27,28,30
7 Mangifera indica Anacardiaceae Aam Gum, Mango peel (Pectin) Binder, Disintegrant, Polymer. 34-37
8 Musa paradisiaca Musaceae Banana Starch, Peel pectin Binder, Disintegrant, Polymer. 38-41
9 Oryza sativa L. Gramineae Bora rice Starch Binder, Disintegrant, Polymer. 44-46
10 Tamarindus indica Fabaceae Tamarind Seed gum Binder, Disintegrant. 49,50
Table 1:
Plants and their parts used as natural excipients.

Solanum tuberosum

Solanum tuberosum, commonly known as potatoes, is a member of the Solanaceae family and is often referred to as the ‘king of vegetables.’ It is the fourth most important food crop in India after rice, wheat, and maize.46 In addition, potatoes have industrial uses such as the production of starch and alcohol. Potato starch, obtained from the root tubers of Solanum tuberosum, is a multifunctional excipient in solid dosage forms, used as a filler/diluent, binding agent, and disintegrating agent.47 Its amylose-amylopectin ratio, crystallinity, and gelatinization properties can strongly affect its swelling and compaction behavior and make it an ideal binder for various solid dosage forms.48 Moreover, potato starch is a sustainable, biodegradable resource that can be modified to obtain products with specific properties.49

Tamarindus indica

Tamarind (Tamarindus indica Linn.), belonging to the Fabaceae family, is a tropical plant found in tropical and subtropical regions. Its sweet-sour pulp is used as food, beverage, and traditional medicine, especially in the African region and India. In traditional medicine, tamarind has been used to treat diarrhea, constipation, fever, and peptic ulcers, as well as to promote wound healing by using its bark and leaves. The tamarind seed gums are used as binders and have been modified by carboxymethylation to improve their binding properties. These modified binders were used to successfully formulate Ibuprofen tablets, with slow dissolution profiles. Raw and chemically modified gums from Tamarindus indica seeds were also evaluated as potent disintegrants and diluents, and tested in sustained-release matrix formulations as a coating agent. Consequently, raw and modified tamarind polysaccharides can be utilized as versatile pharmaceutical excipients in novel drug delivery systems.50

CONCLUSION

This review paper aimed to explore the use of excipients derived from the most common edible natural sources in pharmaceutical formulation development. It was found that natural excipients are becoming increasingly popular due to several advantageous features, such as their abundance, minimal side effects, low toxicity, biocompatibility, patient acceptance, renewable source, and environment-friendly processing. The most commonly used natural sources of excipients, including Dillenia indica, Abelmoschus esculentus, Oryza sativa L, Artocarpus heterophyllus, Tamarindus indica, Musa paradisiaca, Mangifera indica, Ipomoea batatas, Hibiscus sabdariffa, and Solanum tuberosum, have proven to be significant contributors to pharmaceutical formulation design and development.

Cite this article

Sarmah J, Choudhury A, Deka H, Ganguly D, Baishya D, Jyrwa R. A Comprehensive Overview of Edible Natural Excipients and their Potential Use in Pharmaceutical Formulation Development. J Young Pharm. 2023;15(4):589-94.

ACKNOWLEDGEMENT

The author wishes to acknowledge the management of Assam Down town University for proving required facilities to carry out the study.

ABBREVIATIONS

API: Active Pharmaceutical Ingredients
HPMC :Hydroxy propyl methyl cellulose
PEG :Polyethylene Glycol
CL-CMJF :Cross-Linked Carboxymethyl Jackfruit Starch
PVP :Poly Vinyl Pyrrolidine;

References

  1. Arsul VA, Lahoti SR. Natural polysaccharides as pharmaceutical excipients. World J Pharm Res. 2014;3(2):3776-90. [Google Scholar]
  2. Pal RS, Pal Y, Wal A, Wal P. Current review on plant-based pharmaceutical excipients. MEDJ. 2019;6(1):1-5. [CrossRef] | [Google Scholar]
  3. Prabakaran L, Senthil D. Formulation development of patient friendly dosage form: all in one natural excipient as binder, diluents, and disintegrant. Int J Pharm Pharm Sci. 2011;3(S2):97-102. [CrossRef] | [Google Scholar]
  4. Kumar T, Gupta SK, Prajapati MK, Tripathi DK. Natural excipients: a review. Asian J Pharm Life Sci. 2012;2:97-108. [CrossRef] | [Google Scholar]
  5. Kumar P, Singh DP. Pharmaceutical excipients and their role in tablet formulation. Int J Pharm Sci Res. 2013;4(4):1373-81. [CrossRef] | [Google Scholar]
  6. Reddy MR, Manjunath K. Pharmaceutical applications of natural gums, mucilages and pectins – a review. Int J Pharm Chem Sci. 2013;2(3):1233-9. [CrossRef] | [Google Scholar]
  7. Sangwan YS, Sangwan S, Jalwal P, Murti K, Kaushik M. Mucilages and their pharmaceutical applications: an overview. Pharmacol Online. 2011;2:1265-71. [CrossRef] | [Google Scholar]
  8. Shawi AA, Hameed MF, Hussein KA, Thawini HK. Review on the “Biological Applications of Okra Polysaccharides and Prospective Research. Future J Pharm Sci. 2021;7(1):102 [CrossRef] | [Google Scholar]
  9. Rakesh K, Vishal P. Phytochemical, nutritional and pharmacological evidences for . L. J Phytopharmacol. 2016;5(6):238-41. [CrossRef] | [Google Scholar]
  10. Kedar KA, Marakana UV, Chaudhari PD. Evaluation of suspending property of fruit mucilage of . (L) Medie. Res J Pharm Technol. 2010;3(4):1036-8. [CrossRef] | [Google Scholar]
  11. Patil MB, Kumar R, Patil SR, Paschapur MS. Evaluation of disintegrating properties of mucilage. Int J PharmTech Res. 2010;1(2):241-6. [CrossRef] | [Google Scholar]
  12. Gasendo CD, Claire CJ, Pascua SCJ. Cost-effective analysis of the extracted mucilaginous substance of okra () and corn starch as tablet binders, root gatherers. Off J Pharm. 2012;3(1):1-17. [CrossRef] | [Google Scholar]
  13. Choudhary PD, Pawar HA. Recently investigated natural gums and mucilages as pharmaceutical excipients: an overview. J Pharmacol. 2014;1:1-9. [CrossRef] | [Google Scholar]
  14. Baliga MS, Shivashankara AR, Haniadka R, Dsouza J, Bhat HP. Phytochemistry, nutritional and pharmacological properties of Lam (jackfruit): a review. Food Res Int. 2011;44(7):1800-11. [CrossRef] | [Google Scholar]
  15. Manalo RAM, Arollado EC, Pellazar JMM, Siocson MPF, Ramirez RLF. Yellow Linn. and Lam seed starch as binder and disintegrant in paracetamol tablet formulation. J Appl Pharm Sci. 2018;8(03):060-6. [CrossRef] | [Google Scholar]
  16. Koppula T. Isolation of starch from jackfruit seed and evaluation of its binding and disintegrating properties. Pharm Res Bull. 2020;1:1-9. [CrossRef] | [Google Scholar]
  17. Gohain HC, Sahu BP. Formulation and evaluation of mucoadhesive tablet of metformin HCl using jack fruit latex (). Int J Drug Res Tech. Rese Jour of Pharm and Technol. 2016;6(3):182-92. [CrossRef] | [Google Scholar]
  18. Kusuma R, Reddy V, Rao SS. Evaluation of Starch as an Alternative Tablet Excipient to Maize Starch: assessment by Pre formulation and Formulation Studies. Int J Pharm Sci Res. 2015;6(1):57-65. [CrossRef] | [Google Scholar]
  19. Lestari PM, Widayanti A, Afifah H. The effect of pregelatinized taro starch ( (L.) Schott) temperature as filler on thiamine hydrochloride tablet. Herb Pharm Clin Sci. 2019;7(22):827-3832. [CrossRef] | [Google Scholar]
  20. Soni P, Solanki D. Formulation and Evaluation of Sustained Release Matrix Tablet of antiviral Drug by Natural polysaccharide. Int J Chem Tech Res. 2018;11(11):323-8. [CrossRef] | [Google Scholar]
  21. Solanki D, Motiwale M, Mahapatra S. Study of drug release kinetics from sustained release matrix tablets of acyclovir using natural polymer obtained from . Int J Pharm Tech Res. 2020;13(3):172-9. [CrossRef] | [Google Scholar]
  22. Ahmed FAM, Satti NME, Eltahir SE. A Comparative study on some major constituents of karkade ( roselle plant. Int J Life Sci Pharm Res. 2019;9(1):1-12. [CrossRef] | [Google Scholar]
  23. Anel TC, Thokchom R, Subapriya SM, Thokchom J, Singh SS. Array. Int J Adv Res Biol Sci. 2016;3(4):243-8. [CrossRef] | [Google Scholar]
  24. Patil PS, Badgujar SV, Shirsath KG, Sonawane MS. Evaluating the efficacy of Linn Mucilage as Binder in Orodispersible tablets of losartan potassium. J Pharm Adv Res. 2021;4(3):1173-8. [CrossRef] | [Google Scholar]
  25. Frimpong G, Adotey J, Kwakye KO, Kipo SL, Fokuo YD. Potential of aqueous extract of calyces as a coloring agent in three pediatric oral pharmaceutical formulations. J Appl Pharm Sci. 2014;4(12):001-7. [CrossRef] | [Google Scholar]
  26. Shirsand SB, Shivanand SS, Shailashri GG, Keshavshetti G, Jonathan V. Array. Dhaka Univ J Pharm Sci. 2016;15(2):143-9. [CrossRef] | [Google Scholar]
  27. Roullier C, Kambouo R, Paofa J, McKey D, Lebot V. On the origin of sweet potato ( (L.) Lam.) genetic diversity in New Guinea, a secondary center of diversity. Heredity. 2013;110(6):594-604. [PubMed] | [CrossRef] | [Google Scholar]
  28. Djamaan A, Noviza D, Septianingsih D, Suardi M. The use of purple sweet potato () starch as a binder in mangosteen peel extracts lozenges formulation. Pharm Chem. 2016;8(2):410-4. [PubMed] | [CrossRef] | [Google Scholar]
  29. Noerrizki AM, Karuniawan A, Suganda T, Andriani Y, Concibido V, Levita J, et al. Sweet potato ( [L.] Lam.) – A Reviewon its bioprospecting. IOSR JPBS. 2020;15(3):01-7. [PubMed] | [CrossRef] | [Google Scholar]
  30. Jubril I, Jand JM, Mohammed GT. Effects of phosphate modified and pregelatinized sweet potato starches on disintegrant property of paracetamol tablet formulations. J Appl Pharm Sci. 2012;02(02):32-6. [PubMed] | [CrossRef] | [Google Scholar]
  31. Akin-Ajani OD, Itiola OA, Odeku OA. Evaluation of the disintegrant properties of native and modified forms of Fonio and sweet potato starches. Starch Starke. 2016;68(1-2):169-74. [CrossRef] | [Google Scholar]
  32. Mahalia LD, Supriyanto S, Syukri Y. Development of sweet potato ( Lamk.) as an excipient in tablet formulation. J Public Health Res. 2020;9(2):1831 [PubMed] | [CrossRef] | [Google Scholar]
  33. Parvez GM. Pharmacological activities of mango (): a review. J Pharmacogn Phytochem. 2016;5(3):01-7. [PubMed] | [CrossRef] | [Google Scholar]
  34. Jahurul MHA, Zaidul ISM, Ghafoor K, Al-Juhaimi FY, Nyam KL, Norulaini NA, et al. Mango ( L.) by-products, and their valuable components: a review. Food Chem. 2015;183:173-80. [PubMed] | [CrossRef] | [Google Scholar]
  35. Ordu JI, Asuoma NM. Assessment of and corn derived starches on ibuprofen tablet formulation. Int J PharmSci Invent. 2021;10(1):34-41. [PubMed] | [CrossRef] | [Google Scholar]
  36. Malviya R, Srivastava P, Bansal M, Sharma PK. Mango peel pectin as super disintegrating agent. J Sci Ind Res. 2010;69:688-90. [PubMed] | [CrossRef] | [Google Scholar]
  37. Ahmed ESY, Abbas ESE. Extraction and Evaluation of gum as a sustained release polymer in glibenclamide matrix tablets. J Pharm Biosci. 2018;6(4):01-6. [PubMed] | [CrossRef] | [Google Scholar]
  38. Imam MZ, Akter S. Array. J Appl Pharm Sci. 2011;01(05):14-20. [PubMed] | [CrossRef] | [Google Scholar]
  39. Eraga SO, Arhewoh MI, Agboola JO, Iwuagwu MA. Preliminary investigations of banana () starch mucilage as binder in metformin tablet formulation. Pak J Pharm Sci. 2018;31(6):2435-42. [PubMed] | [Google Scholar]
  40. Sandhan S, Thombre N, Aher S. Isolation and Evaluation of starch from Linn. as a Binder in Tablet. IJPSR. 2017;8(8):3484-91. [PubMed] | [Google Scholar]
  41. Babalola OC, Odeku OA. Disintegrant properties of banana starch obtained from the unripe fruits of L. J Appl Pharm Sci. 2014;4(09):083-8. [PubMed] | [Google Scholar]
  42. Osonwa UE, Majekodunmi SO, Onwuzuligbo CC. Potential Use of peel Gum as Adhesive in paracetamol Tablets. AJPSP. 2017;5(1):30-58. [PubMed] | [Google Scholar]
  43. Zaki Ahmad MZ, Akhter S, Dhiman I, Sharma P, Verma R, Rahman M, et al. Tableting properties of Assam bora rice starch. Drug Deliv Lett. 2012;2(1):2-7. [CrossRef] | [Google Scholar]
  44. Shah BH, Hamid FS, Islam S, Ahmed N, Ahmad F, Khan N, et al. Evaluation of elite rice ( L.) lines for yield and yield components. Pakn J Agric Res. 2020;33(1):135 [CrossRef] | [Google Scholar]
  45. Bhattacharya A, Rajak P, Singh A, Sharma N, Kataki MS. Assam bora rice starch as directly compressible filler-binder. Int J Pharm Technol. 2010;2(2):245-54. [CrossRef] | [Google Scholar]
  46. Rajak P, Nath LK, Bhuyan B. Application of Assam Bora rice starch as a binder in formulation of paracetamol tablets. Int J Pharm Pharm Sci. 2015;6(5):118-20. [CrossRef] | [Google Scholar]
  47. Sahair AR, Sneha S, Raghu N, Gopinath TS, Karthikeyan M, Gnanasekaran A, et al. Array. Indian J Phytomed. 2018;10(3):115-24. [CrossRef] | [Google Scholar]
  48. Bayor MT, Tuffour E, Lambon PS. Evaluation of starch from new sweet potato genotypes for use as A pharmaceutical diluent, binder, or disintegrant. J App Pharm Sc. 2013;3(8):S17-23. [CrossRef] | [Google Scholar]
  49. . Array. J Pharmacogn Phytochem. 2016;5(3):50-4. [CrossRef] | [Google Scholar]
  50. Huanbutta K, Sangnim T, Sittikijyothin W. Physicochemical characterization of gum from tamarind seed: potential for pharmaceutical application. Asian J Pharm Sci. 2016;11(1):176-7. [CrossRef] | [Google Scholar]
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