N-Succinylaspart-1-yl Celecoxib is a Potential Colon-Specific Prodrug of Celecoxib with Improved Therapeutic Properties

To develop a colon-specific prodrug of celecoxib, a cyclooxygenase-2 selective inhibitor, which could improve cardiovascular toxicity and therapeutic effectiveness for chemoprevention of colorectal cancer, aspart-1-yl celecoxib (A1C) or aspart-4-yl celecoxib (A4C), succinyl celecoxib (SC), and N-suc...

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Veröffentlicht in:	Journal of pharmaceutical sciences 2012-05, Vol.101 (5), p.1831-1842
Hauptverfasser:	Lee, Yonghyun, Kim, Jeongyun, Kim, Hyunjeong, Kang, Sookjin, Yoon, Jeong-Hyun, Kim, Dae-Duk, Kim, Young Mi, Jung, Yunjin
Format:	Artikel
Sprache:	eng
Schlagworte:	Administration, Oral Animals Aspartic Acid - analogs & derivatives Aspartic Acid - pharmacology Aspartic Acid - therapeutic use Biological and medical sciences cardiovascular toxicity Celecoxib chemoprevention Chromatography, High Pressure Liquid Colon - drug effects colonic drug delivery controlled release/delivery Cyclooxygenase 2 Inhibitors - pharmacology Cyclooxygenase 2 Inhibitors - therapeutic use familial adenomatous polyposis General pharmacology Intestinal Absorption - drug effects Intestine, Small - drug effects Male Medical sciences oral drug delivery Pharmaceutical technology. Pharmaceutical industry Pharmacology. Drug treatments prodrugs Prodrugs - pharmacology Prodrugs - therapeutic use Pyrazoles - pharmacology Pyrazoles - therapeutic use Rats Rats, Sprague-Dawley site-specific delivery Spectrum Analysis - methods Sulfonamides - pharmacology Sulfonamides - therapeutic use
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creator	Lee, Yonghyun Kim, Jeongyun Kim, Hyunjeong Kang, Sookjin Yoon, Jeong-Hyun Kim, Dae-Duk Kim, Young Mi Jung, Yunjin
description	To develop a colon-specific prodrug of celecoxib, a cyclooxygenase-2 selective inhibitor, which could improve cardiovascular toxicity and therapeutic effectiveness for chemoprevention of colorectal cancer, aspart-1-yl celecoxib (A1C) or aspart-4-yl celecoxib (A4C), succinyl celecoxib (SC), and N-succinylaspart-1-yl celecoxib (SA1C) or N-succinylaspart-4-yl celecoxib (SA4C) were prepared and evaluated as a prodrug with such beneficial properties. On incubation with the small intestinal contents while SC, SA1C, and SA4C were stable, A1C and A4C were degraded to liberate celecoxib. In the cecal contents, the other conjugates except for SC and SA4C were cleaved to release celecoxib. These results suggest the colon-specific delivery and activation of SA1C. On oral administration of SA1C or celecoxib, no SA1C was detected in the blood and urine, indicating the limited absorption of SA1C. SA1C delivered a much greater amount of celecoxib to the large intestine while keeping the plasma concentration of celecoxib at much lower level, which is consistent with no change of the serum level of 6-ketoprostaglandin F1α whose decrease is associated with the cardiovascular toxicity of celecoxib. Moreover, SA1C administered orally supplied a greater concentration of celecoxib for the whole colonic tissue. Taken together, SA1C may be a colon-specific prodrug of celecoxib with improved therapeutic properties. © 2012 Wiley Periodicals, Inc. and the American Pharmacists Association J Pharm Sci 101:1831–1842, 2012
doi_str_mv	10.1002/jps.23082
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On incubation with the small intestinal contents while SC, SA1C, and SA4C were stable, A1C and A4C were degraded to liberate celecoxib. In the cecal contents, the other conjugates except for SC and SA4C were cleaved to release celecoxib. These results suggest the colon-specific delivery and activation of SA1C. On oral administration of SA1C or celecoxib, no SA1C was detected in the blood and urine, indicating the limited absorption of SA1C. SA1C delivered a much greater amount of celecoxib to the large intestine while keeping the plasma concentration of celecoxib at much lower level, which is consistent with no change of the serum level of 6-ketoprostaglandin F1α whose decrease is associated with the cardiovascular toxicity of celecoxib. Moreover, SA1C administered orally supplied a greater concentration of celecoxib for the whole colonic tissue. Taken together, SA1C may be a colon-specific prodrug of celecoxib with improved therapeutic properties. © 2012 Wiley Periodicals, Inc. and the American Pharmacists Association J Pharm Sci 101:1831–1842, 2012</description><identifier>ISSN: 0022-3549</identifier><identifier>EISSN: 1520-6017</identifier><identifier>DOI: 10.1002/jps.23082</identifier><identifier>PMID: 22334096</identifier><identifier>CODEN: JPMSAE</identifier><language>eng</language><publisher>Hoboken: Elsevier Inc</publisher><subject>Administration, Oral ; Animals ; Aspartic Acid - analogs & derivatives ; Aspartic Acid - pharmacology ; Aspartic Acid - therapeutic use ; Biological and medical sciences ; cardiovascular toxicity ; Celecoxib ; chemoprevention ; Chromatography, High Pressure Liquid ; Colon - drug effects ; colonic drug delivery ; controlled release/delivery ; Cyclooxygenase 2 Inhibitors - pharmacology ; Cyclooxygenase 2 Inhibitors - therapeutic use ; familial adenomatous polyposis ; General pharmacology ; Intestinal Absorption - drug effects ; Intestine, Small - drug effects ; Male ; Medical sciences ; oral drug delivery ; Pharmaceutical technology. 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Pharm. Sci</addtitle><description>To develop a colon-specific prodrug of celecoxib, a cyclooxygenase-2 selective inhibitor, which could improve cardiovascular toxicity and therapeutic effectiveness for chemoprevention of colorectal cancer, aspart-1-yl celecoxib (A1C) or aspart-4-yl celecoxib (A4C), succinyl celecoxib (SC), and N-succinylaspart-1-yl celecoxib (SA1C) or N-succinylaspart-4-yl celecoxib (SA4C) were prepared and evaluated as a prodrug with such beneficial properties. On incubation with the small intestinal contents while SC, SA1C, and SA4C were stable, A1C and A4C were degraded to liberate celecoxib. In the cecal contents, the other conjugates except for SC and SA4C were cleaved to release celecoxib. These results suggest the colon-specific delivery and activation of SA1C. On oral administration of SA1C or celecoxib, no SA1C was detected in the blood and urine, indicating the limited absorption of SA1C. SA1C delivered a much greater amount of celecoxib to the large intestine while keeping the plasma concentration of celecoxib at much lower level, which is consistent with no change of the serum level of 6-ketoprostaglandin F1α whose decrease is associated with the cardiovascular toxicity of celecoxib. Moreover, SA1C administered orally supplied a greater concentration of celecoxib for the whole colonic tissue. 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Pharmaceutical industry</subject><subject>Pharmacology. Drug treatments</subject><subject>prodrugs</subject><subject>Prodrugs - pharmacology</subject><subject>Prodrugs - therapeutic use</subject><subject>Pyrazoles - pharmacology</subject><subject>Pyrazoles - therapeutic use</subject><subject>Rats</subject><subject>Rats, Sprague-Dawley</subject><subject>site-specific delivery</subject><subject>Spectrum Analysis - methods</subject><subject>Sulfonamides - pharmacology</subject><subject>Sulfonamides - therapeutic use</subject><issn>0022-3549</issn><issn>1520-6017</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2012</creationdate><recordtype>article</recordtype><sourceid>EIF</sourceid><recordid>eNp10M9v0zAUB3ALgVg3OPAPoEiIAwdv_pk4R6igG5tGUYs4Wo79wlzSJNjJuv73GNINDnCyrPd579lfhF5QckoJYWebPp4yThR7hGZUMoJzQovHaJZqDHMpyiN0HOOGEJITKZ-iI8Y4F6TMZ2h3jVejtb7dNyb2JgyY4n2TzaEB2935KvMxM9myG6AdvEmFrulavOrB-trbbBk6F8ZvWVf_1bLzw012se1DdwsuW99AMD2Mw8R7CIOH-Aw9qU0T4fnhPEFfPrxfz8_x1afFxfztFbYiFwwXIFWlnGQsJ4ZWIt0M1I45BzRXklelYASMsKI0paK0Ukq6SkpRVEVdM8VP0KtpbnrNjxHioDfdGNq0UlNJC14KLkRSbyZlQxdjgFr3wW9N2GtK9K-IdYpY_4442ZeHiWO1Bfcg7zNN4PUBmGhNUwfTWh__OKlyRWSZ3Nnkdr6B_f836o_L1f1qPHX4OMDdQ4cJ33Ve8ELqr9cLffn5kr4r87VeJM8nDynhWw9BR-uhteB8ADto1_l_fPAnGaKzew</recordid><startdate>201205</startdate><enddate>201205</enddate><creator>Lee, Yonghyun</creator><creator>Kim, Jeongyun</creator><creator>Kim, Hyunjeong</creator><creator>Kang, Sookjin</creator><creator>Yoon, Jeong-Hyun</creator><creator>Kim, Dae-Duk</creator><creator>Kim, Young Mi</creator><creator>Jung, Yunjin</creator><general>Elsevier Inc</general><general>Wiley Subscription Services, Inc., A Wiley Company</general><general>Wiley</general><general>American Pharmaceutical Association</general><general>Elsevier Limited</general><scope>BSCLL</scope><scope>IQODW</scope><scope>CGR</scope><scope>CUY</scope><scope>CVF</scope><scope>ECM</scope><scope>EIF</scope><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7QO</scope><scope>7QP</scope><scope>7QR</scope><scope>7TK</scope><scope>7U7</scope><scope>8FD</scope><scope>C1K</scope><scope>FR3</scope><scope>P64</scope><scope>RC3</scope></search><sort><creationdate>201205</creationdate><title>N-Succinylaspart-1-yl Celecoxib is a Potential Colon-Specific Prodrug of Celecoxib with Improved Therapeutic Properties</title><author>Lee, Yonghyun ; Kim, Jeongyun ; Kim, Hyunjeong ; Kang, Sookjin ; Yoon, Jeong-Hyun ; Kim, Dae-Duk ; Kim, Young Mi ; Jung, Yunjin</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c4642-7e58b8d52260a1b458baefd2dde16853b9420ea4c49a9811b885db5547b7ff283</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2012</creationdate><topic>Administration, Oral</topic><topic>Animals</topic><topic>Aspartic Acid - analogs & derivatives</topic><topic>Aspartic Acid - pharmacology</topic><topic>Aspartic Acid - therapeutic use</topic><topic>Biological and medical sciences</topic><topic>cardiovascular toxicity</topic><topic>Celecoxib</topic><topic>chemoprevention</topic><topic>Chromatography, High Pressure Liquid</topic><topic>Colon - drug effects</topic><topic>colonic drug delivery</topic><topic>controlled release/delivery</topic><topic>Cyclooxygenase 2 Inhibitors - pharmacology</topic><topic>Cyclooxygenase 2 Inhibitors - therapeutic use</topic><topic>familial adenomatous polyposis</topic><topic>General pharmacology</topic><topic>Intestinal Absorption - drug effects</topic><topic>Intestine, Small - drug effects</topic><topic>Male</topic><topic>Medical sciences</topic><topic>oral drug delivery</topic><topic>Pharmaceutical technology. Pharmaceutical industry</topic><topic>Pharmacology. 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Pharm. Sci</addtitle><date>2012-05</date><risdate>2012</risdate><volume>101</volume><issue>5</issue><spage>1831</spage><epage>1842</epage><pages>1831-1842</pages><issn>0022-3549</issn><eissn>1520-6017</eissn><coden>JPMSAE</coden><abstract>To develop a colon-specific prodrug of celecoxib, a cyclooxygenase-2 selective inhibitor, which could improve cardiovascular toxicity and therapeutic effectiveness for chemoprevention of colorectal cancer, aspart-1-yl celecoxib (A1C) or aspart-4-yl celecoxib (A4C), succinyl celecoxib (SC), and N-succinylaspart-1-yl celecoxib (SA1C) or N-succinylaspart-4-yl celecoxib (SA4C) were prepared and evaluated as a prodrug with such beneficial properties. On incubation with the small intestinal contents while SC, SA1C, and SA4C were stable, A1C and A4C were degraded to liberate celecoxib. In the cecal contents, the other conjugates except for SC and SA4C were cleaved to release celecoxib. These results suggest the colon-specific delivery and activation of SA1C. On oral administration of SA1C or celecoxib, no SA1C was detected in the blood and urine, indicating the limited absorption of SA1C. SA1C delivered a much greater amount of celecoxib to the large intestine while keeping the plasma concentration of celecoxib at much lower level, which is consistent with no change of the serum level of 6-ketoprostaglandin F1α whose decrease is associated with the cardiovascular toxicity of celecoxib. Moreover, SA1C administered orally supplied a greater concentration of celecoxib for the whole colonic tissue. Taken together, SA1C may be a colon-specific prodrug of celecoxib with improved therapeutic properties. © 2012 Wiley Periodicals, Inc. and the American Pharmacists Association J Pharm Sci 101:1831–1842, 2012</abstract><cop>Hoboken</cop><pub>Elsevier Inc</pub><pmid>22334096</pmid><doi>10.1002/jps.23082</doi><tpages>12</tpages></addata></record>
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subjects	Administration, Oral Animals Aspartic Acid - analogs & derivatives Aspartic Acid - pharmacology Aspartic Acid - therapeutic use Biological and medical sciences cardiovascular toxicity Celecoxib chemoprevention Chromatography, High Pressure Liquid Colon - drug effects colonic drug delivery controlled release/delivery Cyclooxygenase 2 Inhibitors - pharmacology Cyclooxygenase 2 Inhibitors - therapeutic use familial adenomatous polyposis General pharmacology Intestinal Absorption - drug effects Intestine, Small - drug effects Male Medical sciences oral drug delivery Pharmaceutical technology. Pharmaceutical industry Pharmacology. Drug treatments prodrugs Prodrugs - pharmacology Prodrugs - therapeutic use Pyrazoles - pharmacology Pyrazoles - therapeutic use Rats Rats, Sprague-Dawley site-specific delivery Spectrum Analysis - methods Sulfonamides - pharmacology Sulfonamides - therapeutic use
title	N-Succinylaspart-1-yl Celecoxib is a Potential Colon-Specific Prodrug of Celecoxib with Improved Therapeutic Properties
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