TY - JOUR
T1 - Analysis of glycoforms and amino acids in infliximab and a biosimilar product using new method with LC/TOF-MS
AU - Tsuda, Masahiro
AU - Otani, Yuki
AU - Yonezawa, Atsushi
AU - Masui, Sho
AU - Ikemi, Yasuaki
AU - Denda, Masaya
AU - Sato, Yuki
AU - Nakagawa, Shunsaku
AU - Omura, Tomohiro
AU - Imai, Satoshi
AU - Nakagawa, Takayuki
AU - Hayakari, Makoto
AU - Matsubara, Kazuo
N1 - Funding Information:
This work was supported by the Research on Regulatory Harmonization and Evaluation of Pharmaceuticals, Medical Devices, Regenerative and Cellular Therapy Products, Gene Therapy Products, and Cosmetics from the Japan Agency for Medical Research and Development, AMED to A.Y., and a Grand-in-Aid for Scientific Research (KAKENHI, 17H06800 to Y.O., 26860102 to M.T.) from the Ministry of Education, Culture, Sports, Science and Technology of Japan.
Publisher Copyright:
© 2018 The Pharmaceutical Society of Japan.
PY - 2018
Y1 - 2018
N2 - Biosimilar products of therapeutic antibodies have been launched all over the world. They can relieve some of the economic burden of medicines. Although clinical trials have demonstrated the equivalency of biosimilar products with their reference product, biosimilar products are not commonly used in clinical practice. One reason is that the structural difference between the reference product and a biosimilar one remains unclear. We analyzed glycoforms and amino acids of an infliximab biosimilar product approved in Japan compared to that of the reference product (Remicade®). By combination of papain digestion and LC/ time-of-flight (TOF)-MS, we established a valuable method to analyze these therapeutic antibodies. Nine glycoforms were detected in infliximab, and a difference in amino acids was observed. In the glycoforms of MMF, MGnF/GnMF, GnGn, GnGnF, AGnF/GnAF, and AAF, the relative intensities were significantly different between the reference and biosimilar product. Furthermore, we elucidated that the content rate of the C-terminal lysine was different among glycoforms. In conclusion, our analytical method can analyze not only amino acids but also carbohydrate chains of therapeutic antibodies, and will provide a useful strategy to evaluate bio-medicines including biosimilar antibodies.
AB - Biosimilar products of therapeutic antibodies have been launched all over the world. They can relieve some of the economic burden of medicines. Although clinical trials have demonstrated the equivalency of biosimilar products with their reference product, biosimilar products are not commonly used in clinical practice. One reason is that the structural difference between the reference product and a biosimilar one remains unclear. We analyzed glycoforms and amino acids of an infliximab biosimilar product approved in Japan compared to that of the reference product (Remicade®). By combination of papain digestion and LC/ time-of-flight (TOF)-MS, we established a valuable method to analyze these therapeutic antibodies. Nine glycoforms were detected in infliximab, and a difference in amino acids was observed. In the glycoforms of MMF, MGnF/GnMF, GnGn, GnGnF, AGnF/GnAF, and AAF, the relative intensities were significantly different between the reference and biosimilar product. Furthermore, we elucidated that the content rate of the C-terminal lysine was different among glycoforms. In conclusion, our analytical method can analyze not only amino acids but also carbohydrate chains of therapeutic antibodies, and will provide a useful strategy to evaluate bio-medicines including biosimilar antibodies.
KW - Biosimilar
KW - Glycosylation
KW - Infliximab
KW - Time-of-flight MS
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U2 - 10.1248/bpb.b18-00491
DO - 10.1248/bpb.b18-00491
M3 - Article
C2 - 30158337
AN - SCOPUS:85055782082
SN - 0918-6158
VL - 41
SP - 1716
EP - 1721
JO - Biological and Pharmaceutical Bulletin
JF - Biological and Pharmaceutical Bulletin
IS - 11
ER -