Analytical Method Development: HPLC Content Uniformity Method – V 2.0

SOP for Development of HPLC Method for Content Uniformity Testing

Department	Analytical Method Development
SOP No.	SOP/AMD/077/2025
Supersedes	SOP/AMD/077/2022
Page No.	Page 1 of 14
Issue Date	19/05/2025
Effective Date	20/05/2025
Review Date	19/05/2026

1. Purpose

This SOP defines the procedure for developing an HPLC-based analytical method for content uniformity testing of solid oral dosage forms. The method ensures that each dosage unit contains the intended

amount of active ingredient within acceptable pharmacopeial limits.

2. Scope

This SOP applies to the Analytical Method Development (AMD) department and covers the HPLC method development activities related to content uniformity analysis for tablets, capsules, and similar dosage forms intended for oral administration.

3. Responsibilities

Analytical Chemist: Executes method development trials, prepares dosage unit samples, and analyzes HPLC data for uniformity.
Reviewer: Validates method suitability based on accuracy, linearity, and precision for individual unit analysis.
QA Officer: Ensures documentation compliance and adherence to ICH and pharmacopeial standards.
Head – AMD: Approves the method for validation and routine content uniformity testing.

4. Accountability

The Head of Analytical Method Development is accountable for ensuring all HPLC methods developed for content uniformity are scientifically sound and meet regulatory and compendial requirements.

5. Procedure

5.1 Pre-Method Development Planning

Review monographs in USP, BP, IP, or existing validated methods.
Assess formulation matrix and potential excipient interferences.
Define acceptance criteria:
- 85% to 115% of label claim for individual units (as per USP <905>)
Document plan in Annexure-1: Method Planning Sheet.

5.2 Chromatographic System Selection

Column: C18, 150 mm × 4.6 mm, 5 µm preferred.
Mobile phase: water with buffer (10–20 mM phosphate or acetate) and organic solvent (ACN or MeOH).
Isocratic or gradient mode depending on matrix complexity and analyte polarity.
Detection wavelength: λmax of API (from UV or PDA scan).
Flow rate: 1.0 mL/min; Injection volume: 10–20 µL.
Record settings in Annexure-2: Chromatographic Parameters Log.

5.3 Sample and Standard Preparation

Standard Preparation:
- Prepare working standard solution using API reference material.
- Concentration to match expected sample level (e.g., 100 µg/mL).
Sample Preparation:
- Individually transfer 10 dosage units into separate volumetric flasks.
- Add diluent, sonicate if required, and bring to volume.
- Filter each solution using 0.45 µm syringe filters.
Document sample coding and prep in Annexure-3: Sample Preparation Log.

5.4 Method Optimization and System Suitability

Inject blank, standard, and individual units (at least 10).
Check:
- Peak symmetry (tailing factor ≤ 2.0)
- Resolution (Rs ≥ 2.0 if multiple components present)
- Retention time reproducibility
Inject standard 5 times; RSD of area ≤ 2.0%.
System suitability must be met before analyzing samples.
Record observations in Annexure-4: System Suitability and Optimization Log.

5.5 Content Uniformity Evaluation

Calculate individual assay content of each unit using:

% Content = (Sample Area / Standard Area) × (Standard Concentration / Sample Concentration) × 100
Report results for each unit and calculate Mean, RSD, and Acceptance Value (AV):
AV = |M – X̄| + k × s
Where:
M = Reference Value (usually target),
X̄ = Mean,
k = Constant (2.4 for 10 units),
s = Standard deviation
Acceptance Criteria (USP <905>): AV ≤ 15.0
Summarize results in Annexure-5: Content Uniformity Calculation Sheet.

5.6 Method Validation Parameters

Linearity: 50–150% of test concentration; R² ≥ 0.999
Accuracy: Recovery from placebo-spiked solution at 80%, 100%, 120% levels
Precision: Repeatability and intermediate precision (RSD ≤ 2.0%)
Specificity: No interference from excipients
Robustness: Small deliberate changes to evaluate consistency
Compile validation data in Annexure-6: Method Validation Summary.

6. Abbreviations

HPLC: High Performance Liquid Chromatography
API: Active Pharmaceutical Ingredient
RSD: Relative Standard Deviation
AV: Acceptance Value
SOP: Standard Operating Procedure

7. Documents

Method Planning Sheet – Annexure-1
Chromatographic Parameters Log – Annexure-2
Sample Preparation Log – Annexure-3
System Suitability and Optimization Log – Annexure-4
Content Uniformity Calculation Sheet – Annexure-5
Method Validation Summary – Annexure-6

8. References

USP <905> – Uniformity of Dosage Units
ICH Q2(R1) – Validation of Analytical Procedures
FDA Guidance for Industry – ANDA: Content Uniformity Studies
USP <621> – Chromatography

9. SOP Version

Version: 2.0

10. Approval Section

	Prepared By	Checked By	Approved By
Signature
Date
Name
Designation
Department

11. Annexures

Annexure-1: Method Planning Sheet

Product	Label Claim	Matrix	Units per Batch	Reference Monograph
XYZ Tablets	50 mg	Lactose-based	10	USP

Annexure-2: Chromatographic Parameters Log

Column	Mobile Phase	Flow Rate	Detection λ	Injection Volume
C18, 150×4.6 mm	60:40 Phosphate buffer:ACN	1.0 mL/min	245 nm	20 µL

Annexure-3: Sample Preparation Log

Unit ID	Sample Code	Dilution Volume	Filtered	Prepared By
Unit 1	CU-001	100 mL	Yes	Sunita Reddy

Annexure-4: System Suitability and Optimization Log

Parameter	Observed Value	Specification	Status
RSD (n=5)	0.72%	≤ 2.0%	Pass

Annexure-5: Content Uniformity Calculation Sheet

Unit	Assay (%)
1	97.8%
2	99.1%
3	100.4%
4	98.5%
5	101.2%
6	96.9%
7	98.7%
8	99.3%
9	100.1%
10	97.5%

Annexure-6: Method Validation Summary

Parameter	Acceptance Criteria	Observed	Status
Linearity	R² ≥ 0.999	0.9994	Pass
Accuracy	98–102%	99.2%	Pass
Precision	RSD ≤ 2.0%	0.86%	Pass

Revision History:

Revision Date	Revision No.	Details	Reason	Approved By
04/05/2025	2.0	Included calculation formulas, AV logic, and expanded annexures	Annual Review