Clinical trial of risedronate in Japanese volunteers: a study on the effects of timing of dosing on absorption

Because of its chemical structure, risedronate was thought to form a complex with divalent cations, e.g., Ca(2+), and to be likely to show changes in the efficiency of absorbance from the gastrointestinal tract according to the presence of food. Therefore, we conducted a crossover study using health...

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Published in	Journal of bone and mineral metabolism Vol. 22; no. 2; pp. 120 - 126
Main Authors	OGURA, Yasuhiko, GONSHO, Akinori, CYONG, Jong-Chol, ORIMO, Hajime
Format	Journal Article
Language	English
Published	Tokyo Springer 01.03.2004 Springer Nature B.V
Subjects	Administration, Oral Adult Biological and medical sciences Calcium Channel Blockers - adverse effects Calcium Channel Blockers - chemistry Calcium Channel Blockers - metabolism Calcium Channel Blockers - therapeutic use Cross-Over Studies Diseases of the osteoarticular system Drug Administration Schedule Eating Etidronic Acid - adverse effects Etidronic Acid - analogs & derivatives Etidronic Acid - chemistry Etidronic Acid - metabolism Etidronic Acid - therapeutic use Humans Intestinal Absorption Japan Male Medical sciences Osteoporosis - drug therapy Risedronate Sodium Time Factors Asia Japan Human Fasting Volunteer Single dose Morning Chemical structure Oral administration Diphosphonic acid derivatives Gastrointestinal Bisphosphonates Japanese Absorption Risedronic acid Food intake Efficiency Digestive diseases Intestinal disease Adult Clinical trial Cations Timing Food
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Abstract	Because of its chemical structure, risedronate was thought to form a complex with divalent cations, e.g., Ca(2+), and to be likely to show changes in the efficiency of absorbance from the gastrointestinal tract according to the presence of food. Therefore, we conducted a crossover study using healthy Japanese adults to examine the effects of food intake on absorption after the oral administration of risedronate and to choose the best timing of regimen for risedronate. Using single doses of 5 mg risedronate, the following four dose times were investigated: (a) in the morning under a fasting condition without breakfast; (b) 30 min before breakfast; (c) 30 min after breakfast; and (d) 3 h after breakfast. The results showed that the C(max) and AUC(0-24) of the plasma risedronate concentrations and its cumulative urinary excretions decreased in the following order: fasting without breakfast >>30 min before breakfast >>3 h after breakfast >>30 min after breakfast. In other words, it was demonstrated that the absorption of risedronate decreases due to the effects of food. Several adverse events, whose causality with risedronate was unknown or possibly related, were observed, including headaches, diarrhea, increased CK-BB, and an increased urinary Beta(2)-microglobulin excretion rate, but none of these events was clinically significant, and none differed in frequency or severity from the events after a single oral administration. In consideration of the optimal practical timings required to administer risedronate for Japanese patients, therefore, it was found that ingesting the drug immediately after waking up in the morning, when the stomach is empty, was optimal, and that it was necessary to refrain from eating and drinking for at least 30 min after drug ingestion. Therefore, we determined that the optimal time for risedronate to be administered in Japanese patients is 30 min before breakfast.
AbstractList	Because of its chemical structure, risedronate was thought to form a complex with divalent cations, e.g., Ca(2+), and to be likely to show changes in the efficiency of absorbance from the gastrointestinal tract according to the presence of food. Therefore, we conducted a crossover study using healthy Japanese adults to examine the effects of food intake on absorption after the oral administration of risedronate and to choose the best timing of regimen for risedronate. Using single doses of 5 mg risedronate, the following four dose times were investigated: (a) in the morning under a fasting condition without breakfast; (b) 30 min before breakfast; (c) 30 min after breakfast; and (d) 3 h after breakfast. The results showed that the C(max) and AUC(0-24) of the plasma risedronate concentrations and its cumulative urinary excretions decreased in the following order: fasting without breakfast >>30 min before breakfast >>3 h after breakfast >>30 min after breakfast. In other words, it was demonstrated that the absorption of risedronate decreases due to the effects of food. Several adverse events, whose causality with risedronate was unknown or possibly related, were observed, including headaches, diarrhea, increased CK-BB, and an increased urinary Beta(2)-microglobulin excretion rate, but none of these events was clinically significant, and none differed in frequency or severity from the events after a single oral administration. In consideration of the optimal practical timings required to administer risedronate for Japanese patients, therefore, it was found that ingesting the drug immediately after waking up in the morning, when the stomach is empty, was optimal, and that it was necessary to refrain from eating and drinking for at least 30 min after drug ingestion. Therefore, we determined that the optimal time for risedronate to be administered in Japanese patients is 30 min before breakfast. Because of its chemical structure, risedronate was thought to form a complex with divalent cations, e.g., Ca^sup 2+^, and to be likely to show changes in the efficiency of absorbance from the gastrointestinal tract according to the presence of food. Therefore, we conducted a crossover study using healthy Japanese adults to examine the effects of food intake on absorption after the oral administration of risedronate and to choose the best timing of regimen for risedronate. Using single doses of 5mg risedronate, the following four dose times were investigated: (a) in the morning under a fasting condition without breakfast; (b) 30min before breakfast; (c) 30min after breakfast; and (d) 3h after breakfast. The results showed that the C^sub max^ and AUC^sub 0-24^ of the plasma risedronate concentrations and its cumulative urinary excretions decreased in the following order: fasting without breakfast 30min before breakfast 3h after breakfast 30min after breakfast. In other words, it was demonstrated that the absorption of risedronate decreases due to the effects of food. Several adverse events, whose causality with risedronate was unknown or possibly related, were observed, including headaches, diarrhea, increased CK-BB, and an increased urinary Β^sub 2^-microglobulin excretion rate, but none of these events was clinically significant, and none differed in frequency or severity from the events after a single oral administration. In consideration of the optimal practical timings required to administer risedronate for Japanese patients, therefore, it was found that ingesting the drug immediately after waking up in the morning, when the stomach is empty, was optimal, and that it was necessary to refrain from eating and drinking for at least 30min after drug ingestion. Therefore, we determined that the optimal time for risedronate to be administered in Japanese patients is 30min before breakfast.[PUBLICATION ABSTRACT]
Author	CYONG, Jong-Chol GONSHO, Akinori OGURA, Yasuhiko ORIMO, Hajime
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Keywords	Human Fasting Volunteer Single dose Morning Chemical structure Oral administration Diphosphonic acid derivatives Gastrointestinal Bisphosphonates Japanese Absorption Risedronic acid Food intake Efficiency Digestive diseases Intestinal disease Adult Clinical trial Cations Timing Food
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Snippet	Because of its chemical structure, risedronate was thought to form a complex with divalent cations, e.g., Ca(2+), and to be likely to show changes in the... Because of its chemical structure, risedronate was thought to form a complex with divalent cations, e.g., Ca^sup 2+^, and to be likely to show changes in the...
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SubjectTerms	Administration, Oral Adult Biological and medical sciences Calcium Channel Blockers - adverse effects Calcium Channel Blockers - chemistry Calcium Channel Blockers - metabolism Calcium Channel Blockers - therapeutic use Cross-Over Studies Diseases of the osteoarticular system Drug Administration Schedule Eating Etidronic Acid - adverse effects Etidronic Acid - analogs & derivatives Etidronic Acid - chemistry Etidronic Acid - metabolism Etidronic Acid - therapeutic use Humans Intestinal Absorption Japan Male Medical sciences Osteoporosis - drug therapy Risedronate Sodium Time Factors
Title	Clinical trial of risedronate in Japanese volunteers: a study on the effects of timing of dosing on absorption
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