Lyophilization and Development of Solid Protein Pharmaceuticals

Overview

Journal Int J Pharm

Specialties Chemistry
Pharmacology

Date 2000 Sep 1

PMID 10967427

Citations 212

Authors

W Wang

Affiliations

Soon will be listed here.

Abstract

Developing recombinant protein pharmaceuticals has proved to be very challenging because of both the complexity of protein production and purification, and the limited physical and chemical stability of proteins. To overcome the instability barrier, proteins often have to be made into solid forms to achieve an acceptable shelf life as pharmaceutical products. The most commonly used method for preparing solid protein pharmaceuticals is lyophilization (freeze-drying). Unfortunately, the lyophilization process generates both freezing and drying stresses, which can denature proteins to various degrees. Even after successful lyophilization with a protein stabilizer(s), proteins in solid state may still have limited long-term storage stability. In the past two decades, numerous studies have been conducted in the area of protein lyophilization technology, and instability/stabilization during lyophilization and long-term storage. Many critical issues have been identified. To have an up-to-date perspective of the lyophilization process and more importantly, its application in formulating solid protein pharmaceuticals, this article reviews the recent investigations and achievements in these exciting areas, especially in the past 10 years. Four interrelated topics are discussed: lyophilization and its denaturation stresses, cryo- and lyo-protection of proteins by excipients, design of a robust lyophilization cycle, and with emphasis, instability, stabilization, and formulation of solid protein pharmaceuticals.

Citing Articles

Understanding dry proteins and their protection with solid-state hydrogen-deuterium exchange.

Brom J, Pielak G Protein Sci. 2025; 34(3):e70075.

PMID: 39998978 PMC: 11854353. DOI: 10.1002/pro.70075.

Lyophilized human platelet lysate: manufacturing, quality control, and application.

Wendland K, Koblin L, Stobbe D, Dahms A, Singer D, Bekeschus S Front Cell Dev Biol. 2025; 13:1513444.

PMID: 39931242 PMC: 11807961. DOI: 10.3389/fcell.2025.1513444.

Formulation development and feasibility of AAV5 as a lyophilized drug product.

Vargas S, Sharifi F, Nambayan R, Moshashaee S, Siahaan T J Pharm Sci. 2025; 114(2):1214-1223.

PMID: 39827914 PMC: 11844822. DOI: 10.1016/j.xphs.2025.01.004.

Designed miniproteins potently inhibit and protect against MERS-CoV.

Ragotte R, Tortorici M, Catanzaro N, Addetia A, Coventry B, Froggatt H bioRxiv. 2024; .

PMID: 39574666 PMC: 11580849. DOI: 10.1101/2024.11.03.621760.

The Role of Phase Separation and Local Mobility in the Stabilization of a Lyophilized IgG2 Formulation.

Lay-Fortenbery A, Holcomb R, Henry C, Manning M, Munson E AAPS PharmSciTech. 2024; 25(8):268.

PMID: 39562383 DOI: 10.1208/s12249-024-02984-7.