Mina Tsurumi scite author profile

Mina Tsurumi

5Publications

9Citation Statements Received

98Citation Statements Given

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Affiliations

Sanofi (Mexico), Sanofi (Japan)

Publications

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Long-term safety and efficacy of agalsidase beta in Japanese patients with Fabry disease: aggregate data from two post-authorization safety studies

Tsurumi

Suzuki

Hokugo

et al. 2021

Expert Opinion on Drug Safety

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Background: Enzyme replacement therapy in Fabry disease has been available in Japan since 2004. Two post-authorization safety studies were conducted to evaluate agalsidase beta in Japanese patients with Fabry disease in real-world practice.Research Design and Methods: The Special Drug Use Investigation monitored the long-term safety and efficacy of agalsidase beta, and the Drug Use Investigation monitored safety in patients not participating in the Special Drug Use Investigation. Safety and efficacy evaluations included adverse drug reactions (ADRs), infusion-associated reactions and hypersensitivity reactions, and change in blood GL-3 level over time. Results: Of 396 patients in the aggregated data set, safety and efficacy analysis sets comprised 307 and 196 patients, respectively. ADRs occurred in 93 (30.3%) patients and serious ADRs occurred in 25 (8.1%) patients, with general disorders and administration site conditions (n=55, 17.9%), nervous system disorders (n=30, 9.8%) and skin and subcutaneous tissue disorders (n=23, 7.5%) the most common.Reductions in blood GL-3 levels occurred over the study, irrespective of age or disease phenotype. Conclusions: Agalsidase beta demonstrated acceptable safety and tolerability, with sustained reductions in blood GL-3 levelsin Japanese patients with Fabry disease in real-world clinical practice Clinical Trial Registration: NCT00233870/AGAL03004 (Special Drug Use Investigation of Agalsidase beta) ARTICLE HISTORY

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A survey on the patient journey in Fabry disease in Japan

Tsurumi

Ozaki

Eto³

2022

Molecular Genetics and Metabolism Reports

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Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: post-hoc analysis of a Japanese post-marketing study

Lee¹,

Tsurumi²,

Eto³

2023

Orphanet J Rare Dis

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Background Agalsidase beta, an enzyme replacement therapy for Fabry disease, is dosed biweekly at 1 mg/kg body weight, with increasing infusion rates based on tolerability. The US label specifies ≥ 90-min infusions for all patients; the US and EU labels require ≤ 15 mg/hr infusions in patients < 30 kg. The Japanese label allows infusions up to 30 mg/hr, allowing < 90-min dosing for some patients weighing < 45 kg. Japanese post-marketing data were analyzed for rate of infusion-associated reactions (IARs), adverse events (AEs), and serious AEs (SAEs) based on infusion rate and patient attributes (weight, antibody status). Results Data were available for 436 reduced-duration infusions (< 90 min) and 2242 standard infusions (≥ 90 min). SAEs were rare (0.6%), and the frequency of all safety events decreased over the treatment course. Little impact of infusion duration on safety outcomes was observed: IARs and AEs were numerically more common when infusion duration was ≥ 90 min compared to < 90 min (IARs: 2.0% vs 0.9%; AEs: 2.9% vs 1.4%), while the rate of SAEs was similar (0.4% vs 0.5%). IAR, AE, and SAE frequencies decreased significantly with increasing infusion rates, and this trend was consistent in patients < 30 kg. Safety events tended to be less frequent in patients < 30 kg vs those ≥ 30 kg (IARs: 1.8% vs 2.1%; AEs: 2.3% vs 3.6%; SAEs: 0.0% vs 0.6%), although the differences were not statistically significant. IARs occurred in < 1% of all infusions in the < 30 kg group, 84% of which were < 90 min. More anti-agalsidase beta antibody-positive patients experienced IARs (41.9% vs 30.7%; P = 0.0445) and AEs (61.1% vs 49.3%; P = 0.0497) vs antibody-negative patients; however, there was no significant difference in the frequency of SAEs. In patients with available data, no changes in antibody status were observed after infusion durations were reduced to < 90 min. Conclusions The results of this post-hoc analysis demonstrated no significant impact of infusion duration on safety outcomes, and no significant difference in outcomes between patients of different weights. These findings suggest that infusion times in patients who are tolerating treatment can, with careful monitoring, be gradually decreased.

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Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: Evidence from a Japanese post-marketing study

Eto¹,

Lee²,

Tsurumi³

2023

Molecular Genetics and Metabolism

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Cholera Acidosis and Its Therapy

Tsurumi¹

1922

Arch Intern Med

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Acidosis is now generally known to be present in various diseases, such as diabetes, nephritis, uremia, and when violent diarrhea and vomiting occur clinically, there is also a rapid decrease in the body fluids. In most cases of cholera, the victim falls into a state of temporary inanition, and in consequence of the action of the toxin on the kidneys, so-called cholera nephritis very often develops. The decrease of blood alkali and the accumulation of acid in the body, make the existence of acidosis a certainty. Sellards noted the remarkable tolerance of the urine to alkali, while

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Mina Tsurumi

Long-term safety and efficacy of agalsidase beta in Japanese patients with Fabry disease: aggregate data from two post-authorization safety studies

A survey on the patient journey in Fabry disease in Japan

Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: post-hoc analysis of a Japanese post-marketing study

Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: Evidence from a Japanese post-marketing study

Cholera Acidosis and Its Therapy

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Mina Tsurumi

Long-term safety and efficacy of agalsidase beta in Japanese patients with Fabry disease: aggregate data from two post-authorization safety studies

A survey on the patient journey in Fabry disease in Japan

Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: post-hoc analysis of a Japanese post-marketing study

Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: Evidence from a Japanese post-marketing study

Cholera Acidosis and Its Therapy

Contact Info

Product

Resources

About

Safety and tolerability of agalsidase beta infusions shorter than 90 min in patients with Fabry disease: Evidence from a Japanese post-marketing study