Synthesis and biologic properties of hydrophilic sapphyrins, a new class of tumor-selective inhibitors of gene expression

doi:10.1186/1476-4598-6-9

. 2007 Jan 19:6:9.

doi: 10.1186/1476-4598-6-9.

Synthesis and biologic properties of hydrophilic sapphyrins, a new class of tumor-selective inhibitors of gene expression

Zhong Wang¹, Philip S Lecane, Patricia Thiemann, Qing Fan, Cecilia Cortez, Xuan Ma, Danielle Tonev, Dale Miles, Louie Naumovski, Richard A Miller, Darren Magda, Dong-Gyu Cho, Jonathan L Sessler, Brian L Pike, Samantha M Yeligar, Mazen W Karaman, Joseph G Hacia

Affiliations

PMID: 17233922
PMCID: PMC1784109
DOI: 10.1186/1476-4598-6-9

Synthesis and biologic properties of hydrophilic sapphyrins, a new class of tumor-selective inhibitors of gene expression

Zhong Wang et al. Mol Cancer. 2007.

. 2007 Jan 19:6:9.

doi: 10.1186/1476-4598-6-9.

Authors

Affiliation

¹ Pharmacyclics, Inc., Sunnyvale, California, USA. zwang@pcyc.com

PMID: 17233922
PMCID: PMC1784109
DOI: 10.1186/1476-4598-6-9

Abstract

Background: Sapphyrin analogues and related porphyrin-like species have attracted attention as anticancer agents due to their selective localization in various cancers, including hematologic malignancies, relative to surrounding tissues. Sapphyrins are electron affinic compounds that generate high yields of singlet oxygen formation. Although initially explored in the context of photodynamic therapy, sapphyrins have intrinsic anticancer activity that is independent of their photosensitizing properties. However, the mechanisms for their anticancer activity have not been fully elucidated.

Results: We have prepared a series of hydrophilic sapphyrins and evaluated their effect on proliferation, uptake, and cell death in adherent human lung (A549) and prostate (PC3) cancer cell lines and in an A549 xenograft tumor model. PCI-2050, the sapphyrin derivative with the highest in vitro growth inhibitory activity, significantly lowered 5-bromo-2'-deoxyuridine incorporation in S-phase A549 cells by 60% within eight hours and increased levels of reactive oxygen species within four hours. The growth inhibition pattern of PCI-2050 in the National Cancer Institute 60 cell line screen correlated most closely using the COMPARE algorithm with known transcriptional or translational inhibitors. Gene expression analyses conducted on A549 plateau phase cultures treated with PCI-2050 uncovered wide-spread decreases in mRNA levels, which especially affected short-lived transcripts. Intriguingly, PCI-2050 increased the levels of transcripts involved in RNA processing and trafficking, transcriptional regulation, and chromatin remodeling. We propose that these changes reflect the activation of cellular processes aimed at countering the observed wide-spread reductions in transcript levels. In our A549 xenograft model, the two lead compounds, PCI-2050 and PCI-2022, showed similar tumor distributions despite differences in plasma and kidney level profiles. This provides a possible explanation for the better tolerance of PCI-2022 relative to PCI-2050.

Conclusion: Hydrophilic sapphyrins were found to display promise as novel agents that localize to tumors, generate oxidative stress, and inhibit gene expression.

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Figures

**Figure 1**
Effect of sapphyrins on cell proliferation. A, Structure of sapphyrins. B, A549 and C, PC3 cancer cells were treated with inhibitors for 24 hours, medium was replaced, and relative proliferation measured after an additional 48 hours by tetrazolium salt reduction. The anti-proliferative activity of cisplatin is shown for comparison.

**Figure 2**
Biological effects of sapphyrins on A549 lung cancer cells. A, 5-Bromo-2'-deoxyuridine (BrdU) incorporation after exposure to PCI-2050 at indicated concentrations. The effect of actinomycin D (ActD, 200 ng/mL) treatment is shown for comparison. B, Cells were treated with inhibitors for 24 hours, medium was replaced, and viability measured after an additional 48 hours by propidium iodide staining. C, Cells were treated with sapphyrins for 4 hours, washed, and sapphyrin uptake estimated by cellular fluorescence above 650 nm. D, Cells were treated with PCI-2050 at indicated concentrations for 4 hours, washed, treated with dichlorofluorescin diacetate, and dichlorofluorescein fluorescence (DCF) measured in live-gated cells. Effect of hydrogen peroxide (H₂O₂, 200 μM), actinomycin D (Act D, 5 μg/mL), and pretreatment with L-buthionein- [S,R]-sulfoximine (BSO, 100 μM) for 24 hours are shown for comparison.

**Figure 3**
Hierarchical clustering analysis of gene expression data from drug-treated A549 cell cultures. The dendrograms were generated based on average linkage hierarchical clustering of expression data from 422 probe tilings whose coefficient of variation was greater than 0.15 across all groups. Data from untreated (mannitol) and drug-treated [(sapphyrin PCI-2050 = 2050) or (actinomycin D = ActD)] A549 cultures are provided in triplicate using the noted concentrations. The relative expression levels (↑ = up-regulated, ↓ = down-regulated) of selected gene groupings in drug-treated versus control cells are provided on the right side of the figure. Note that this reflects relationships only within the subset of genes used for cluster analysis.

**Figure 4**
Activity of sapphyrins in A549 tumor xenograft model. A, Median tumor volume (± SEM) over time in mice treated with control (5% mannitol) vehicle, cisplatin (4 mg/kg q.d. × 4 i.p.), PCI-2050 (10 μmol/kg qd × 2 i.v.), or PCI-2022 (20 μmol/kg qd × 2 i.v.). * p < 0.001. B, Log concentration of PCI-2022 and PCI-2050 in plasma (μM) or in kidney and tumor (nmol/g) over time is shown.

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References

1. Bauer VJ, Clive DLJ, Dolphin D, Paine JB, III, Harris FL, King MM, Loder J, Wang SWC, Woodward RB. Sapphyrins: Novel Aromatic Pentapyrrolic Macrocycles. j am chem soc. 1983;105:6429–6436. doi: 10.1021/ja00359a012. - DOI
1. Broadhurst MJ, Grigg R, Johnson AW. Synthesis of 22-Pi-Electron Macrocycles, Sapphyrins and Related Compounds. J Chem Soc, Perkin Trans. 1972;1:2111–2116. doi: 10.1039/p19720002111. - DOI
1. Sessler J, Cyr MJ, Lynch V, McGhee E, Ibers JA. Synthetic and Structural Studies of Sapphyrin, a 22-Pi-Electron Pentapyrrolic "Expanded Porphyrin". j am chem soc. 1990;112:2810–2813. doi: 10.1021/ja00163a059. - DOI
1. Sessler JL, Davis JM. Sapphyrins: versatile anion binding agents. Acc Chem Res. 2001;34:989–997. doi: 10.1021/ar980117g. - DOI - PubMed
1. Springs SL, Gosztola D, Wasielewski M, Kral V, Andreivsky A, Sessler JL. Picosecond Dynamics of Energy Transfer in Porphyrin-Sapphyrin Noncovalent Assemblies. j am chem soc. 1999;121:2281–2289. doi: 10.1021/ja9835436. - DOI

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[1] Bauer VJ, Clive DLJ, Dolphin D, Paine JB, III, Harris FL, King MM, Loder J, Wang SWC, Woodward RB. Sapphyrins: Novel Aromatic Pentapyrrolic Macrocycles. j am chem soc. 1983;105:6429–6436. doi: 10.1021/ja00359a012. - DOI

[2] Bauer VJ, Clive DLJ, Dolphin D, Paine JB, III, Harris FL, King MM, Loder J, Wang SWC, Woodward RB. Sapphyrins: Novel Aromatic Pentapyrrolic Macrocycles. j am chem soc. 1983;105:6429–6436. doi: 10.1021/ja00359a012. - DOI

[3] Broadhurst MJ, Grigg R, Johnson AW. Synthesis of 22-Pi-Electron Macrocycles, Sapphyrins and Related Compounds. J Chem Soc, Perkin Trans. 1972;1:2111–2116. doi: 10.1039/p19720002111. - DOI

[4] Broadhurst MJ, Grigg R, Johnson AW. Synthesis of 22-Pi-Electron Macrocycles, Sapphyrins and Related Compounds. J Chem Soc, Perkin Trans. 1972;1:2111–2116. doi: 10.1039/p19720002111. - DOI

[5] Sessler J, Cyr MJ, Lynch V, McGhee E, Ibers JA. Synthetic and Structural Studies of Sapphyrin, a 22-Pi-Electron Pentapyrrolic "Expanded Porphyrin". j am chem soc. 1990;112:2810–2813. doi: 10.1021/ja00163a059. - DOI

[6] Sessler J, Cyr MJ, Lynch V, McGhee E, Ibers JA. Synthetic and Structural Studies of Sapphyrin, a 22-Pi-Electron Pentapyrrolic "Expanded Porphyrin". j am chem soc. 1990;112:2810–2813. doi: 10.1021/ja00163a059. - DOI

[7] Sessler JL, Davis JM. Sapphyrins: versatile anion binding agents. Acc Chem Res. 2001;34:989–997. doi: 10.1021/ar980117g. - DOI - PubMed

[8] Sessler JL, Davis JM. Sapphyrins: versatile anion binding agents. Acc Chem Res. 2001;34:989–997. doi: 10.1021/ar980117g. - DOI - PubMed

[9] Springs SL, Gosztola D, Wasielewski M, Kral V, Andreivsky A, Sessler JL. Picosecond Dynamics of Energy Transfer in Porphyrin-Sapphyrin Noncovalent Assemblies. j am chem soc. 1999;121:2281–2289. doi: 10.1021/ja9835436. - DOI

[10] Springs SL, Gosztola D, Wasielewski M, Kral V, Andreivsky A, Sessler JL. Picosecond Dynamics of Energy Transfer in Porphyrin-Sapphyrin Noncovalent Assemblies. j am chem soc. 1999;121:2281–2289. doi: 10.1021/ja9835436. - DOI

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Synthesis and biologic properties of hydrophilic sapphyrins, a new class of tumor-selective inhibitors of gene expression

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Synthesis and biologic properties of hydrophilic sapphyrins, a new class of tumor-selective inhibitors of gene expression

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