Tumor priming enhances siRNA delivery and transfection in intraperitoneal tumors

Jie Wang; Ze Lu; Bertrand Z Yeung; M Guillaume Wientjes; David J Cole; Jessie L-S Au

doi:10.1016/j.jconrel.2014.01.012

Tumor priming enhances siRNA delivery and transfection in intraperitoneal tumors

J Control Release. 2014 Mar 28:178:79-85. doi: 10.1016/j.jconrel.2014.01.012. Epub 2014 Jan 23.

Authors

Jie Wang¹, Ze Lu¹, Bertrand Z Yeung², M Guillaume Wientjes², David J Cole³, Jessie L-S Au⁴

Affiliations

¹ Optimum Therapeutics LLC, 9363 Towne Centre Drive, Suite 110, San Diego 92121, USA.
² Optimum Therapeutics LLC, 9363 Towne Centre Drive, Suite 110, San Diego 92121, USA; College of Pharmacy, The Ohio State University, Columbus 43210, USA.
³ Medical University of South Carolina, Charleston 29425, USA.
⁴ Optimum Therapeutics LLC, 9363 Towne Centre Drive, Suite 110, San Diego 92121, USA; College of Pharmacy, The Ohio State University, Columbus 43210, USA; Medical University of South Carolina, Charleston 29425, USA. Electronic address: jau@optimumtx.com.

Abstract

Cancers originating from the digestive system account for 290,000 or ~20% of all new cancer cases annually in the US. We previously developed paclitaxel-loaded tumor-penetrating microparticles (TPM) for intraperitoneal (IP) treatment of peritoneal tumors (Lu et al., 2008; Tsai et al., 2007; Tsai et al., 2013). TPM is undergoing NIH-supported IND-enabling studies for clinical evaluation. The present study evaluated the hypothesis that TPM, via inducing apoptosis and expanding the interstitial space, promotes the delivery and transfection of lipid vectors containing siRNA. The in vivo model was the metastatic human Hs766T pancreatic tumor that, upon IP injection, produced widely distributed solid tumors and ascites in the peritoneal cavity in 100% of animals. The target gene was survivin, an anti-apoptotic protein induced by chemotherapy and associated with metastases and poor prognosis of patients with gastric and colorectal cancers. The siRNA carrier was pegylated liposomes comprising cationic and neutral lipids plus a fusogenic lipid (PCat). PCat-loaded with survivin siRNA (PCat-siSurvivin) was active in cultured cells (decreased survivin mRNA and protein levels, reduced cell clonogenicity, enhanced paclitaxel activity), but lost its activity in vivo; this difference is consistent with the well-known problem of inadequate delivery and transfection of siRNA in vivo. In comparison, single agent TPM prolonged animal survival and, as expected, induced survivin expression in tumors. Addition of PCat-siSurvivin reversed the TPM-induced survivin expression and enhanced the antitumor activity of TPM. The finding that in vivo survivin knockdown by PCat-siSurvivin was successful only when it was given in combination with TPM provides the proof-of-concept that tumor priming promotes the delivery and transfection of liposomal siRNA. The data further suggest the TPM/PCat-siSurvivin combination as a potentially useful chemo-gene therapy for peritoneal cancer.

Keywords: Intraperitoneal chemotherapy; Microparticles; Paclitaxel; Pancreatic cancer; Peritoneal carcinomatosis; siRNA.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Antineoplastic Agents, Phytogenic / administration & dosage*
Antineoplastic Agents, Phytogenic / pharmacokinetics
Cell Line, Tumor
Combined Modality Therapy
Female
Humans
Inhibitor of Apoptosis Proteins / genetics
Inhibitor of Apoptosis Proteins / metabolism
Liposomes
Mice
Mice, Nude
Paclitaxel / administration & dosage*
Paclitaxel / pharmacokinetics
Peritoneal Neoplasms / metabolism
Peritoneal Neoplasms / therapy*
RNA, Small Interfering / administration & dosage*
RNA, Small Interfering / pharmacokinetics
Survivin
Transfection
Xenograft Model Antitumor Assays

Substances

Antineoplastic Agents, Phytogenic
BIRC5 protein, human
Inhibitor of Apoptosis Proteins
Liposomes
RNA, Small Interfering
Survivin
Paclitaxel

Abstract

Publication types

MeSH terms

Substances

Grants and funding