AI Article Synopsis

  • Antiangiogenic agents have been a common treatment for advanced HCC, while embolization with cytostatic drugs is preferred for intermediate cases; this study explores combining these treatments for improved intraarterial delivery.
  • The research involved loading drug-eluting beads with different drugs, including doxorubicin and sunitinib, and analyzing their loading, release dynamics, and impact on cellular proliferation against an HCC cell line.
  • Results showed that doxorubicin can be effectively combined with antiangiogenic drugs, demonstrating satisfactory drug loading and favorable release behaviors that inhibit HCC cell growth in vitro.

Article Abstract

Purpose: Antiangiogenic agents have been used for many years as a first-line systemic treatment for advanced HCC. Embolization with cytostatic drugs on the other hand is the first-line treatment for intermediate HCC. The two types of drugs have not been combined for intraarterial delivery yet. The loading and release dynamics and the in vitro effect of their combination are tested in this experimental study.

Materials And Methods: Drug-eluting beads were loaded with doxorubicin, sunitinib and sunitinib analogue piperazine (SAP) alone and with their combinations. Diameter change, loading, release, and effect in cellular proliferation were assessed.

Results: The average microsphere diameter after loading was 473.7 µm (μm) for Doxorubicin, 388.4 μm for Sunitinib, 515.5 μm for SAP, 414.8 μm for the combination Doxorubicin/Sunitinib and 468.8 μm for the combination Doxorubicin /SAP. Drug release in 0.9% NaCl was 10% for Doxorubicin, 49% for Sunitinib, 25% for SAP, 20%/18% for the combination Doxorubicin/Sunitinib, and 18%/23% for the combination Doxorubicin/SAP whereas in human plasma it was 56%, 27%, 13%, 76%/63% and 62%/15%, respectively. The mean concentration of Doxorubicin that led to inhibition of 50% of cellular proliferation in an HCC Huh7 cell line was 163.1 nM (nM), for Sunitinib 10.3 micromolar (μΜ), for SAP 16.7 μΜ, for Doxorubicin/Sunitinib 222.4 nM and for Doxorubicin/SAP 275 nM.

Conclusions: Doxorubicin may be combined with antiangiogenic drugs with satisfactory in vitro loading and release outcomes and effect on cellular lines.

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Source
http://dx.doi.org/10.1007/s00270-024-03714-zDOI Listing

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