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Pharmaceutical Alternatives: Polymorphic Form-Related and Particle Size-Related Therapeutic Nonequivalence01:27

Pharmaceutical Alternatives: Polymorphic Form-Related and Particle Size-Related Therapeutic Nonequivalence

Changes in polymorphic forms can significantly influence the bioavailability of poorly soluble drugs. Although the FDA defines pharmaceutical equivalence based on having the same active ingredient, dosage form, and route of administration, it does not automatically disqualify products with different polymorphic forms. This means two products with different polymorphs can still be deemed pharmaceutically equivalent. However, polymorphic differences can affect properties like wettability,...
Pharmaceutical Alternatives: Stability-Related Therapeutic Nonequivalence01:22

Pharmaceutical Alternatives: Stability-Related Therapeutic Nonequivalence

Generic intravenous (IV) drugs are considered bioequivalent to their branded counterparts due to their 100% bioavailability upon administration. However, variations in stability among different drug products can significantly influence their therapeutic performance, even if they are pharmaceutically equivalent.Cefuroxime, a prophylactic antimicrobial, is often used as a single-dose IV injection for patients undergoing coronary artery bypass grafting surgery. A 3 g dose typically provides...
Formulation and Manufacturing Process: Physical Attributes of Generic Tablets and Capsules01:18

Formulation and Manufacturing Process: Physical Attributes of Generic Tablets and Capsules

Bioequivalence in generic drugs, such as tablets and capsules, refers to their pharmaceutical equivalence to the brand-name counterparts. However, for therapeutic equivalence, manufacturers must also consider physical attributes like size, shape, and weight (FDA Guidance for Industry, December 2003). Discrepancies in these aspects could impact patient compliance and cause medication errors. For instance, swallowing difficulties, often experienced with larger tablets or capsules, can lead to...
Pharmaceutical Alternatives: Excipients and Impurities-Related Therapeutic Nonequivalence01:19

Pharmaceutical Alternatives: Excipients and Impurities-Related Therapeutic Nonequivalence

Pharmaceutical products contain more than just the active drug; they also contain various excipients such as binders, solubilizers, stabilizers, preservatives, and other elements. In some cases, impurities or contaminants might be present. Traditionally, quality control in pharmaceuticals has primarily focused on the analysis of the active drug, often overlooking the impact of these additional components. The recent issue with heparin contamination by over-sulfated chondroitin sulfate, a...
Bioequivalence of Drugs: Drugs with Multiple Indications01:09

Bioequivalence of Drugs: Drugs with Multiple Indications

The concept of therapeutic equivalence (TE) in drugs with multiple indications is complex. A generic drug may be therapeutically equivalent to a brand-name product for one specific indication, but this doesn't necessarily mean it's equivalent for all other indications. Evidence of TE in one patient group and bioequivalence shown in healthy volunteers can support—but not confirm—TE for other indications. However, definitive proof requires individual clinical studies for each indication due to...
Drug Dissolution: Requirements and Profile Comparison01:14

Drug Dissolution: Requirements and Profile Comparison

The acceptance criteria for dissolution profile data are anchored in Q values, representing the percentage of drug dissolved within a specified period. This assessment unfolds in three stages:First Stage: The test passes if all six drug dosage units are equal to or greater than Q plus 5%; otherwise, the sample proceeds to the second stage.Second Stage: The average of twelve units must be equal to or greater than Q, with no unit falling below Q - 15% to pass; if not, it progresses to the final...

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Related Experiment Video

Updated: Jul 8, 2026

Characteristics of Precipitation-formed Polyethylene Glycol Microgels Are Controlled by Molecular Weight of Reactants
11:32

Characteristics of Precipitation-formed Polyethylene Glycol Microgels Are Controlled by Molecular Weight of Reactants

Published on: December 23, 2013

Differences in taste between two polyethylene glycol preparations.

Maria M Szojda1, Chris J J Mulder, Richelle J F Felt-Bersma

  • 1Department of Gastroenterology and Hepatology, University Medical Centre, Amsterdam, P.O. Box 7057, 1007 MB Amsterdam, The Netherlands.

Journal of Gastrointestinal and Liver Diseases : JGLD
|January 15, 2008
PubMed
Summary

Polyethylene glycol (PEG) 4000 was found to taste significantly better than PEG 3350 in a study comparing the two common constipation treatments. This finding may improve patient compliance and treatment effectiveness for chronic constipation.

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Microwave-assisted Functionalization of Poly(ethylene glycol) and On-resin Peptides for Use in Chain Polymerizations and Hydrogel Formation

Published on: October 29, 2013

Taste Exam: A Brief and Validated Test
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Taste Exam: A Brief and Validated Test

Published on: August 17, 2018

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Last Updated: Jul 8, 2026

Characteristics of Precipitation-formed Polyethylene Glycol Microgels Are Controlled by Molecular Weight of Reactants
11:32

Characteristics of Precipitation-formed Polyethylene Glycol Microgels Are Controlled by Molecular Weight of Reactants

Published on: December 23, 2013

Microwave-assisted Functionalization of Poly(ethylene glycol) and On-resin Peptides for Use in Chain Polymerizations and Hydrogel Formation
15:33

Microwave-assisted Functionalization of Poly(ethylene glycol) and On-resin Peptides for Use in Chain Polymerizations and Hydrogel Formation

Published on: October 29, 2013

Taste Exam: A Brief and Validated Test
07:10

Taste Exam: A Brief and Validated Test

Published on: August 17, 2018

Area of Science:

  • Gastroenterology
  • Pharmacology
  • Clinical Trials

Background:

  • Polyethylene glycol (PEG) preparations are widely used for chronic constipation in adults and children.
  • Patient compliance is often hindered by poor taste, leading to therapy failure.
  • Two common PEG formulations, PEG 4000 and PEG 3350, have differing taste profiles.

Purpose of the Study:

  • To compare the taste acceptability of PEG 4000 versus PEG 3350.
  • To evaluate the impact of taste on potential patient compliance in constipation management.

Main Methods:

  • A double-blind, cross-over randomized trial involving 100 volunteers.
  • Participants tasted both PEG 4000 and PEG 3350 preparations without swallowing, followed by a mouth rinse.
  • Taste was assessed using a 5-point scoring scale for each preparation.

Main Results:

  • PEG 4000 received a significantly higher mean taste score (3.9) compared to PEG 3350 (2.7) (p<0.0001).
  • The order of tasting influenced the perception of PEG 3350, but not PEG 4000.
  • No significant differences in taste preference were observed based on gender or age.

Conclusions:

  • PEG 4000 demonstrates superior taste compared to PEG 3350.
  • Improved taste of PEG 4000 may enhance patient compliance and treatment efficacy for chronic constipation.