Biological and Pharmaceutical Bulletin
The Pharmaceutical Society of Japan, established in 1880, is one of Japan’s oldest and most distinguished academic societies. The Society currently has around 15,000 members. It publishes three monthly scientific journals. Chemical and Pharmaceutical Bulletin (Chem. Pharm. Bull.) began publication in 1953 as Pharmaceutical Bulletin. It covers chemistry fields in the pharmaceutical and health sciences. Biological and Pharmaceutical Bulletin (Biol. Pharm. Bull.) began publication in 1978 as the Journal of Pharmacobio-Dynamics, which then merged the Journal of Health Science, another former Society’s journal, in 2012. It covers various biological topics in the pharmaceutical and health sciences. Yakugaku Zasshi (Japanese for “Pharmaceutical Science Journal”) has the longest history, with publication beginning in 1881. Yakugaku Zasshi is published mostly in Japanese, except for some articles related to clinical pharmacy and pharmaceutical education, which are published in English. The main aim of the Society’s journals is to advance the pharmaceutical sciences with research reports, scientific communication, and high-quality discussion. The average review time for articles submitted to the journals is around one month for first decision. The complete texts of all of the Society’s journals can be freely accessed through J-STAGE. The Society’s editorial committee hopes that the content of its journals will be useful to your research, and also invites you to submit your own work to the journals.

Chairman of Committee
Hidehiko Nakagawa
Graduate School of Pharmaceutical Sciences, Nagoya City University
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11,779 registered articles
(updated on October 14, 2025)
Online ISSN : 1347-5215
Print ISSN : 0918-6158
ISSN-L : 0918-6158
1.7
2024 Journal Impact Factor (JIF)
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Featured article
Volume 48 (2025) Issue 8 Pages 1191-1198
Enhancement of Immune Modulation by Toll-Like Receptor 9 Adjuvant Combination Subcutaneous Immunotherapy for Japanese Cedar Pollinosis Read more
Editor's pick

This study showed the potential to enhance the efficacy and safety of Allergy immunotherapy (AIT) with Japanese cedar pollen (JCP) using a prophylactic mouse model of allergic sensitization. The co-immunization with JCP extract, K3 CpG oligodeoxynucleotide (CpG-ODN) and di-lauryl phosphatidylcholine/deoxycholic acid (DLPC/DA) micelles in naïve mice suppressed the T-helper 2 immune response and the reduction of allergen-specific IgE, increased allergen-specific IgG2a levels. These immunomodulatory effects were accompanied by the suppression of airway inflammation and sneezing frequency. These data suggested the combination of K3 CpG-ODN and DLPC/DA micelles with JCP immunization could potentially serve as a next-generation AIT treatment regimen for JC pollinosis.

Volume 48 (2025) Issue 8 Pages 1199-1206
Evaluation of Transport Activity Using Mouse Jejunal Epithelial Cell Monolayer Culture System Read more
Editor's pick

The authors developed a rapid and easy method for culturing a monolayer of epithelial cells isolated from mouse jejunal crypts. Using this system, they evaluated changes in the transport activity of P-gp and Pept1, as well as the mRNA expression levels of P-gp, Pept1, and Cyp3a11-representative transporters expressed in the small intestine. The functions of P-gp and Pept1 were validated using specific inhibitors. Calcitriol treatment modulated the expression of P-gp and Cyp3a11 but not Pept1. Overall, this monolayer culture system is a useful research tool for assessing the activity and expression variability of transporters.

Volume 48 (2025) Issue 8 Pages 1224-1232
Comparative Proteomic Analysis of Endocytic Cell-Surface Proteins in Vascular and Lymphatic Endothelial Cells Read more
Editor's pick

In this study, Ito et al. provide a comprehensive proteomic comparison of endocytic cell-surface proteins in human vascular and lymphatic endothelial cells. Through cell-surface biotinylation, internalization assays, and SWATH-MS–based quantitative proteomics, the authors identified unique sets of proteins that define the specific functions of each endothelial cell type. Vascular endothelial cells were enriched in proteins linked to angiogenesis, nutrient uptake, and metabolism. In contrast, lymphatic endothelial cells displayed proteins associated with immune regulation and extracellular matrix organization. These findings underscore endothelial heterogeneity and pinpoint promising molecular targets for selective drug delivery and imaging.

Volume 48 (2025) Issue 8 Pages 1233-1238
In Silico Exploration of Therapeutics for GLP-1 Receptor Agonist-Induced Nausea and Their in Vivo Validation in Mice Read more
Editor's pick

[Highlighted Paper selected by Editor-in-Chief]  
Despite their efficacy, GLP-1 receptor agonists, antidiabetic and antiobestic drugs, frequently induce nausea and vomiting, which are prominent factors for non-adherence to these drugs. In this study, Shibui et al. explored the FDA Adverse Event Reporting System database to determine the effective drug combinations that mitigate GLP-1 receptor agonist-induced nausea and vomiting in real-world settings. They further investigated the effects of the identified drugs on GLP-1 receptor agonist-induced pica behavior, a behavioral index of nausea in mice. Through these analyses in silico and in vivo, they identified gabapentin as a possible therapeutic against GLP-1 receptor agonist-induced nausea and vomiting. 

Volume 48 (2025) Issue 8 Pages 1246-1254
Guanidinylated Chitosan as a Multifunctional Enhancer for Improved Flurbiprofen Delivery Read more
Editor's pick

This study evaluated guanidinylated chitosan (GCS), a modified derivative of low-molecular-weight chitosan (CS), as an oral excipient to improve poorly water-soluble drugs. Flurbiprofen (FP) was used as a model drug in kneaded dispersions with GCS (FP-GCS) or CS (FP-CS). Both polymers increased FP solubility, but FP-GCS significantly enhanced dissolution in water and gastric fluid. In rats, FP-GCS achieved higher plasma concentrations, indicating improved gastrointestinal permeability, and markedly reduced gastric ulceration. These findings suggest that GCS enhances both the bioavailability and gastrointestinal safety of FP.

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Announcements from publisher
  • Data Presentation Guidelines
    The data should be prepared in accordance with the guidelines.https://bpb.pharm.or.jp/document/Guidelines_DP_BPB.pdf
  • Biol. Pharm. Bull. Vol. 48 No. 9
    Current Topics: Current Status of Cancer Diagnosis and Treatment
  • 2024 Announcement of Academic Journals’ Awards Biological and Pharmaceutical Bulletin (BPB)https://bpb.pharm.or.jp/award/bpb_award.pdf
  • Biol. Pharm. Bull. Vol. 48 No. 3
    Current Topics: Recent Advances in Antibacterial Resistance by Japanese Pharmaceutical Scientists
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