More Peptide. Fewer IPCs.
Continuous Polishing Chromatography with MCSGP.

Bachem — a leading global peptide and oligonucleotide CDMO — integrated MCSGP into large-scale peptide API manufacturing at Bubendorf, Switzerland. The original process used 2D batch chromatography with extensive side-cut recycling (nearly 20% of all runs were side-cuts) to achieve a purity target of >99.3%. MCSGP delivered the same purity with significantly better process economics and throughput.

Results vs. batch for a production-scale peptide:

• Purity: >99.3% maintained — fully comparable to batch
• Material consumption (PMI) reduced 70% — from 5,700 to 1,600 kg per kg API
• Processing time: 5 days → 24 hours
• Lyophilization volume reduced ~50%
• IPC analyses reduced ~75%
• Side-cut re-chromatography completely eliminated
• Crude throughput approximately 3× higher per day with 2×30 cm columns vs. equivalent batch

Source: Bachem AG — “Reducing Solvent Consumption for Large-Scale Peptide API Manufacturing” (Case Study, June 2023)

A landmark open-access collaboration between Bachem AG and YMC ChromaCon presents the first regulatory-compliant Process Characterization (PC) and Process Performance Qualification (PPQ) approach for MCSGP — directly supporting FDA/EMA filings for therapeutics manufactured using continuous chromatography.

Molecule: Bivalirudin (20-mer synthetic peptide), PC on Contichrom CUBE 30, PPQ on Contichrom TWIN 500 with 2×30 cm i.D. columns.

PPQ campaign results (54.5 kg crude, 4 multiday runs):

• Yield: 62% gross-to-gross (+5 pp vs. legacy batch); effective yield 76%
• IPC burden reduced 96% (81 IPCs/kg → 3.2 IPCs/kg)
• PMI reduced 73% (~5,200 → 1,400 kg/kg)
• Output: 33.6 kg API at 99.2% purity across all 397 elutions

This publication provides a regulatory roadmap for any peptide or oligonucleotide manufacturer seeking FDA/EMA process validation.

Eisenhuth, R.; Müller-Späth, T. Processes, 2025, 13(12), 3950. DOI: 10.3390/pr13123950 (Open Access)

Molecule: Glucagon (29 amino acids, MW 3485 Da), crude synthetic mixture (55% chromatographic purity in feed) Equipment: Contichrom CUBE Combined (ChromaCon/YMC) Mode: RP-HPLC — Daisogel-SP-120-10-C8-Bio, 10 µm; mobile phases: ammonium acetate/ACN gradient

Key finding: MCSGP increased glucagon recovery by +23% at identical purity (~89%) — from 71.2% to 87.7% — demonstrating that even a process designed from a single batch chromatogram, with no dedicated optimisation, meaningfully improves yield. The 38% productivity reduction is an inherent tradeoff of the interconnected phases; for expensive therapeutic peptides like glucagon, maximising recovery more than compensates for this. The MCSGP process ran fully automated for 5 cycles (steady state achieved after cycle 1), illustrating the method-transfer simplicity of the ChromIQ® MCSGP Wizard workflow.

De Luca, C., Felletti, S., Lievore, G. et al. J. Chromatogr. A, 1625, 461304 (2020). DOI: 10.1016/j.chroma.2020.461304

A: MCSGP continuously recycles the impure side-fractions that batch RP-HPLC discards — recovering peptide product without compromising purity. For production-scale peptides, Bachem reported +21% yield. Published data on glucagon showed +23%, and improvements of +10–50% are typical depending on the complexity of the impurity profile.

Yes. MCSGP uses the same reversed-phase (C18, C8, C4), ion exchange, and mixed-mode stationary phases and eluent systems as your existing batch method. No change to your resin or buffer chemistry is needed — MCSGP process parameters are then developed from those existing conditions, typically within 1–2 weeks on the CUBE.

Peptides with complex impurity profiles see the largest gains — particularly long-chain GLP-1 agonists (semaglutide, tirzepatide), peptidomimetics, and multi-modified sequences. Even well-optimized short peptides like glucagon and icatibant show meaningful yield improvements.

Yes. Bachem has run GMP MCSGP peptide production since 2022 at their Bubendorf facility. A December 2025 landmark publication (Müller-Späth et al., Processes 13(12), 3950) provides the first-ever Process Characterization and PPQ framework — demonstrated on the 20-mer peptide Bivalirudin.

Yes. All Contichrom® systems support batch, 2D/3D integrated batch, and continuous modes on the same hardware. The TWIN HPLC production systems are dual-mode (MCSGP + batch) on a single skid — so you can run both processes without separate equipment.

Starting from an existing batch RP-HPLC or IEX method, the ChromIQ® software wizard enables a first MCSGP peptide run within approximately one day. Full optimization typically takes 1–2 weeks.

AutoPeak® monitors the peptide elution profile in real-time via UV and conductivity, dynamically adjusting collection windows to compensate for crude feed variability, column aging, and retention time drift — enabling robust, unattended 24/7 peptide purification. It has been validated as a Process Analytical Technology (PAT).

For peptide manufacturing, MCSGP requires up to 75% less solvent, 50% less lyophilization volume, and smaller upstream SPPS batches (from higher yield) — dramatically improving Process Mass Intensity (PMI). The FDA actively encourages this shift to continuous manufacturing for pharmaceutical APIs.