Inorganics (Jun 2024)

The Synthesis and Pharmacokinetics of a Novel Liver-Targeting Cholic Acid-Conjugated Carboplatin in Rats

  • Yinyin Lan,
  • Fuguo Han,
  • Anli Gao,
  • Xuemei Fan,
  • Yanli Hao,
  • Zhao Wang,
  • Weiping Liu,
  • Jing Jiang,
  • Qingfei Liu

DOI
https://doi.org/10.3390/inorganics12070184
Journal volume & issue
Vol. 12, no. 7
p. 184

Abstract

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A novel cholic acid-conjugated carboplatin (CP-CA) is developed as a liver-targeting prodrug of carboplatin (CP) for liver cancer. Instead of using CP as a raw material, CP-CA was synthesized simultaneously. This paper is focused on the comparison of CP-CA and CP with respect to their pharmacokinetic (PK) and tissue distribution profiles in rats after their intravenous administration. Additionally, their uptake by human liver tumor cell Huh7 and normal human liver cell HL7702 are investigated. The inductively coupled plasma mass spectrometry (ICP-MS) method is applied for the determination of platinum in plasma, tissues, and cells. The PK results show that both the AUC0–t and AUC0–∞ data on Pt for CP-CA are significantly higher than those for CP (p 1, Vd1, and Vd2 data on Pt for CP-CA are significantly lower than those for CP (p 0–t is significantly higher (p 0–t and AUC0–∞ of Pt for CP-CA compared to for CP. The tissue distribution results show that CP-CA is mainly distributed and accumulated in the liver after its intravenous administration to rats, revealing its liver-targeting profile. Compared to CP, CP-CA is more easily taken up by human liver cancer cells and normal human liver cells. The results suggest that CP-CA has a potential for further development as a new prodrug specific to liver cancer.

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