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dc.contributor.authorChang, Ya-Huien_US
dc.contributor.authorChen, Chiao-Yunen_US
dc.contributor.authorSingh, Gyanen_US
dc.contributor.authorChen, Hsing-Yinen_US
dc.contributor.authorLiu, Gin-Chungen_US
dc.contributor.authorGoan, Yih-Gangen_US
dc.contributor.authorAime, Silvioen_US
dc.contributor.authorWang, Yun-Mingen_US
dc.date.accessioned2014-12-08T15:12:07Z-
dc.date.available2014-12-08T15:12:07Z-
dc.date.issued2011-02-21en_US
dc.identifier.issn0020-1669en_US
dc.identifier.urihttp://dx.doi.org/10.1021/ic101799cen_US
dc.identifier.urihttp://hdl.handle.net/11536/9288-
dc.description.abstractThe present study was designed to exploit optimum lipophilicity and high water-exchange rate (k(ex)) on low molecular weight Gd(III) complexs to generate high bound relaxivity (r(1)(b)), upon binding to the lipophilic site of human serum albumin (HSA). Two new carbon backbone modified TTDA (3,6,10-tri(carboxymethyl)-3,6,10-triazadodecanedioic acid) derivatives, CB-TTDA and Bz-CB-TTDA, were synthesized. The complexes [Gd(CB-TTDA)(H(2)O)](2-) and [Gd(Bz-CB-TTDA)(H(2)O)](2-) both display high stability constant (log K(GdL) = 20.28 and 20.09, respectively). Furthermore, CB-TTDA (log K((Gd/Zn)) = 4.22) and Bz-CB-TTDA (log K((Gd/Zn)) = 4.12) exhibit superior selectivity of Gd(III) against Zn(II) than those of TTDA (log K((Gd/Zn)) = 2.93), EPTPA-bz-NO(2) (log K((Gd/Zn)) = 3.19), and DTPA (log K((Gd/Zn)) = 3.76). However, the stability constant values of [Gd(CB-TTDA)(H(2)O)](2-) and [Gd(Bz-CB-TTDA)(H(2)O)](2-) are lower than that of MS-325. The parameters that affect proton relaxivity have been determined in a combined variable temperature (17)O NMR and NMRD study. The water exchange rates are comparable for the two complexes, 232 x 10(6) s(-1) for [Gd(CB-TTDA)(H(2)O)](2-) and 271 x 10(6) s(-1) for [Gd(Bz-CB-TTDA)(H(2)O)](2-). They are higher than those of [Gd(TTDA)(H(2)O)](2-) (146 x 10(6) s(-1)), [Gd(DTPA)(H(2)O)](2-) (4.1 x 10(6) s(-1)), and MS-325 (6.1 x 10(6) s(-1)). Elevated stability and water exchange rate indicate that the presence of cyclobutyl on the carbon backbone imparts rigidity and steric constraint to [Gd(CB-TTDA)(H(2)O)](2-) and [Gd(Bz-CB-TTDA)(H(2)O)](2-). In addition, the major objective for selecting the cyclobutyl is to tune the lipophilicity of [Gd(Bz-CB-TTDA)(H(2)O)](2-). The binding affinity of [Gd(Bz-CB-TTDA)(H(2)O)](2-) to HSA was evaluated by ultrafiltration study across a membrane with a 30 kDa MW cutoff, and the first three stepwise binding constants were determined by fitting the data to a stoichiometric model. The binding association constants (K(A)) for [Gd(CB-TTDA)(H(2)O)](2-) and [Gd(Bz-CB-TTDA)(H(2)O)](2-) are 1.1 x 10(2) and 1.5 x 10(3), respectively. Although the K(A) value for [Gd(Bz-CB-TTDA)(H(2)O)](2-) is lower than that of MS-325 (K(A) = 3.0 x 10(4)), the r(1)(b) value, r(1)(b) = 66.7 mM(-1) s(-1) for [Gd(Bz-CB-TTDA)(H(2)O)](2-), is significantly higher than that of MS-325 (r(1)(b) = 47.0 mM(-1) s(-1)). As measured by the Zn(II) transmetalation process, the kinetic stabilities of [Gd(CB-TTDA)(H(2)O)](2-), [Gd(Bz-CB-TTDA)(H(2)O)](2-), and [Gd(DTPA)(H(2)O)](2-) are similar and are significantly higher than that of [Gd(DTPA-BMA)(H(2)O)](2-) High thermodynamic and kinetic stability and optimized lipophilicity of [Gd(CB-TTDA)(H(2)O)](2-) make it a favorable blood pool contrast agent for MRI.en_US
dc.language.isoen_USen_US
dc.titleSynthesis and Physicochemical Characterization of Carbon Backbone Modified [Gd(TTDA)(H(2)O)](2-) Derivativesen_US
dc.typeArticleen_US
dc.identifier.doi10.1021/ic101799cen_US
dc.identifier.journalINORGANIC CHEMISTRYen_US
dc.citation.volume50en_US
dc.citation.issue4en_US
dc.citation.spage1275en_US
dc.citation.epage1287en_US
dc.contributor.department分子醫學與生物工程研究所zh_TW
dc.contributor.departmentInstitute of Molecular Medicine and Bioengineeringen_US
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