Phase 1 Study of Weekly Polyethylene Glycol-Camptothecin in Patients with Advanced Solid Tumors and Lymphomas

Posey, James; Saif, Muhammad Wasif; Carlisle, Ricarda; Goetz, Andrew; Rizzo, Jinee; Stevenson, Suzanne; Rudoltz, Marc S.; Kwiatek, Joseph; Simmons, Paul; Rowinsky, Eric K.; Takimoto, Chris H.; Tolcher, Anthony W.

doi:10.1158/1078-0432.ccr-05-0783

Cited by 47 publications

(23 citation statements)

References 14 publications

(16 reference statements)

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“…This high binding to human albumin is not observed with the active metabolic of irinotecan, SN-38 (30,31). When CPT was conjugated to linear PEG, the PK profiles of the released CPT in animals (32) and humans (33,34) showed the same form of the dynamics as observed for CRLX101. Likewise, the MAG-CPT gave released CPT dynamics of the same type (35,36).…”

Section: Discussionmentioning

confidence: 81%

Correlating preclinical animal studies and human clinical trials of a multifunctional, polymeric nanoparticle

Eliasof

Lazarus

Peters

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

124

119

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Nanoparticles are currently being investigated in a number of human clinical trials. As information on how nanoparticles function in humans is difficult to obtain, animal studies that can be correlative to human behavior are needed to provide guidance for human clinical trials. Here, we report correlative studies on animals and humans for CRLX101, a 20-to 30-nm-diameter, multifunctional, polymeric nanoparticle containing camptothecin (CPT). CRLX101 is currently in phase 2 clinical trials, and human data from several of the clinical investigations are compared with results from multispecies animal studies. The pharmacokinetics of polymer-conjugated CPT (indicative of the CRLX101 nanoparticles) in mice, rats, dogs, and humans reveal that the area under the curve scales linearly with milligrams of CPT per square meter for all species. Plasma concentrations of unconjugated CPT released from CRLX101 in animals and humans are consistent with each other after accounting for differences in serum albumin binding of CPT. Urinary excretion of polymer-conjugated CPT occurs primarily within the initial 24 h after dosing in animals and humans. The urinary excretion dynamics of polymer-conjugated and unconjugated CPT appear similar between animals and humans. CRLX101 accumulates into solid tumors and releases CPT over a period of several days to give inhibition of its target in animal xenograft models of cancer and in the tumors of humans. Taken in total, the evidence provided from animal models on the CRLX101 mechanism of action suggests that the behavior of CRLX101 in animals is translatable to humans.nanomedicine | clinical translation | interspecies scaling | pharmacodynamics | Nanoparticles

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Section: Discussionmentioning

confidence: 81%

Correlating preclinical animal studies and human clinical trials of a multifunctional, polymeric nanoparticle

Eliasof

Lazarus

Peters

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

124

119

View full text Add to dashboard Cite

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“…The 20-OH of CPT in Pegamotecan, is blocked by the alaninate linker, which stabilizes the CPT molecule into its active lactone conformation [57]. The MTD of Pegamotecan when administered weekly for 3 of 4 weeks was 3,240 mg/m 2 , with neutropenia being its DLT [58]. Other grade 3 and 4 toxic effects were anemia, thrombocytopenia, fatigue, prolonged partial thromboplastin time, hemorrhagic cystitis, dysuria, and urinary frequency.…”

Section: Peg-camptothecin (Pegamotecan) and Peg-sn38 (Ezn-2208)mentioning

confidence: 99%

Polymer-drug conjugates: Recent development in clinical oncology

Wallace

2008

Advanced Drug Delivery Reviews

395

237

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Targeted drug delivery aims to increase the therapeutic index by making more drug molecules available at the diseased sites while reducing systemic drug exposure. In this update, we provide an overview of polymer-drug conjugates that have advanced into the clinical trials. These systems use synthetic water-soluble polymers as the drug carriers. The preclinical pharmacology and recent data in clinical trials with poly(L-glutamic acid)-paclitaxel (PG-TXL) are discussed first. This is followed by a summary of conjugates of a variety of polymeric conjugates with chemotherapeutic agents. Results from early clinical trials of these polymer-drug conjugates have demonstrated several advantages over the corresponding parent drugs, including fewer side effects, enhanced therapeutic efficacy, ease of drug administration, and improved patient compliance. Collectively, these data warrant further clinical development of polymer-drug conjugates as a new class of anticancer agents.

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“…Polyglutamic acid (PGA)-paclitaxel copolymer (CT-2103) (Xyotax) is entering the market as cancer treatment for non-small-cell lung cancer in women (Singer 2005). Polyethyleneglycol in conjugation with camptothecin (EZ-246, Pegamotecan) (Posey et al 2005) and cyclodextrin in conjugation with camptothecin (Schluep et al 2006a, b;Zamboni et al 2006) are entering clinical trials. Polymer-drug conjugates are being directed not only against tumour cells, but also against angiogenic blood vessels, for example, HPMA-fumagillol (TNP-470) caplostatin (Satchi-Fainaro et al 2004;Huang et al 2004;Inoue et al 2003;Bhujwalla et al 2003), the HPMA copolymer-RGD4C-Tc-99m conjugate, capable of targeting tumour angiogenic vessels and delivering adequate radiotherapy to arrest tumour growth (Mitra et al 2006) and PEGylated cyclic arginine-glycine-aspartic acid (RGD) radiotracers (64-Cu-DOTAPEG-RGD and 125 I-RGD-mPEG) targeted at integrins (Chen et al 2004a, b).…”

Section: Polymersmentioning

confidence: 99%

Molecular imaging with nanoparticles: giant roles for dwarf actors

Debbage

Jaschke

2008

Histochem Cell Biol

230

212

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Molecular imaging, first developed to localise antigens in light microscopy, now encompasses all imaging modalities including those used in clinical care: optical imaging, nuclear medical imaging, ultrasound imaging, CT, MRI, and photoacoustic imaging. Molecular imaging always requires accumulation of contrast agent in the target site, often achieved most efficiently by steering nanoparticles containing contrast agent into the target. This entails accessing target molecules hidden behind tissue barriers, necessitating the use of targeting groups. For imaging modalities with low sensitivity, nanoparticles bearing multiple contrast groups provide signal amplification. The same nanoparticles can in principle deliver both contrast medium and drug, allowing monitoring of biodistribution and therapeutic activity simultaneously (theranostics). Nanoparticles with multiple bioadhesive sites for target recognition and binding will be larger than 20 nm diameter. They share functionalities with many subcellular organelles (ribosomes, proteasomes, ion channels, and transport vesicles) and are of similar sizes. The materials used to synthesise nanoparticles include natural proteins and polymers, artificial polymers, dendrimers, fullerenes and other carbon-based structures, lipid-water micelles, viral capsids, metals, metal oxides, and ceramics. Signal generators incorporated into nanoparticles include iron oxide, gadolinium, fluorine, iodine, bismuth, radionuclides, quantum dots, and metal nanoclusters. Diagnostic imaging applications, now appearing, include sentinal node localisation and stem cell tracking.

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Phase 1 Study of Weekly Polyethylene Glycol-Camptothecin in Patients with Advanced Solid Tumors and Lymphomas

Cited by 47 publications

References 14 publications

Correlating preclinical animal studies and human clinical trials of a multifunctional, polymeric nanoparticle

Correlating preclinical animal studies and human clinical trials of a multifunctional, polymeric nanoparticle

Polymer-drug conjugates: Recent development in clinical oncology

Molecular imaging with nanoparticles: giant roles for dwarf actors

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