Multicomponent assembly of 4-aza-podophyllotoxins: A fast entry to highly selective and potent anti-leukemic agents

European Journal of Medicinal Chemistry

Volumn 106, Issue , 2015, Pages 167-179

  Jeedimalla, Nagalakshmi ^a   Flint, Madison ^a   Smith, Lyndsay ^b   Haces, Alberto ^a   Minond, Dmitriy ^b,c   Roche, Stéphane P ^a  

^a FLORIDA ATLANTIC UNIVERSITY   (United States)

^b TORREY PINES INSTITUTE FOR MOLECULAR STUDIES   (United States)

^c AUBURN UNIVERSITY   (United States)

Author keywords

AML; Anti leukemic agents; Aza podophyllotoxins; Etoposide; Multicomponent reactions; SAR study

Indexed keywords

10 (3,4,5-TRIMETHOXYPHENYL) 3,6,7,8 TETRAHYDRO 1H CYCLOPENTA[G]FURO[3,4 B]QUINOL; 10 (PERFLUOROPHENYL) 3,4,6,7,8,10 HEXAHYDRO 1H CYCLOPENTA[G]FURO[3,4 B]QUINOLIN 1 ONE; 10 HENYL 3,4,6,7,8,10 HEXAHYDRO 1H CYCLOPENTA[G]FURO[3,4B]QUINOLIN 1 ONE; 11 (3,4,5 TRIMETHOXYPHENYL) 4,6,7,8,9,11 HEXAHYDROBENZO[G] FURO[3,4 B]QUINOLIN 1(3H)ONE; 11 (3,4,5 TRIMETHOXYPHENYL) 6,7,8,9 TETRAHYDROBENZO[G]FURO [3,4 B]QUINOLIN 1(3H)ONE; 11 (PERFLUOROPHENYL) 4,6,7,8,9,11 HEXAHYDROBENZO[G]FURO[3,4 B]QUINOLIN 1(3H)ONE; 11 PHENYL 4,6,7,8,9,11 HEXAHYDROBENZO[G]FURO[3,4 B]QUINOLIN 1(3H)ONE; 5 (METHYLTHIO) 9 (3,4,5 TRIMETHOXYPHENYL) 4,9 DIHYDROFURO [3,4 B]QUINOLIN 1(3H)ONE; 6 (DIFLUOROMETHOXY) 9 (3,4,5 TRIMETHOXYPHENYL) 4,9 DIHYDROFURO[3,4 B]QUINOLIN 1(3H)ONE; 6 (DIFLUOROMETHOXY) 9 (PERFLUOROPHENYL) 4,9 DIHYDROFURO[3,4 B]QUINOLIN 1(3H)ONE; 6 (DIFLUOROMETHOXY) 9 PHENYL 4,9 DIHYDROFURO[3,4 B]QUINOLIN 1(3H)ONE; 6 (METHYLTHIO) 9 (3,4,5 TRIMETHOXYPHENYL) 4,9 DIHYDROFURO [3,4 B]QUINOLIN 1(3H)ONE; 6 (METHYLTHIO) 9 (PERFLUOROPHENYL) 4,9 DIHYDROFURO[3,4 B] QUINOLIN 1(3H)ONE; 6 HYDROXY 9 (4 HYDROXY 3 METHOXYPHENYL) 4,9 DIHYDROFURO[3,4 B]QUINOLIN 1(3H)ONE; 7 (3,4,5 TRIMETHOXYPHENYL) 7,11 DIHYDROBENZO[H]FURO[3,4 B] QUINOLIN 8(10H)ONE; 7 (BENZO[D][1,3]DIOXOL 5 YL) 8 OXO 7,8,10,11 TETRAHYDROBENZO[H]FURO[3,4 B]QUINOLINE 5 CARBONITRILE; 7 (PERFLUOROPHENYL) 7,11 DIHYDROBENZO[H]FURO[3,4 B]QUINOLIN 8(10H)ONE; 8 OXO 7 (3,4,5 TRIMETHOXYPHENYL) 7,8,10,11 TETRAHYDROBENZO[H]FURO[3,4 B]QUINOLINE 5 CARBONITRILE; 8 OXO 7 (PERFLUOROPHENYL) 7,8,10,11 TETRAHYDROBENZO[H]FURO [3,4 B]QUINOLINE 5 CARBONITRILE; 9 (2,3 DIMETHOXYPHENYL) 6 (METHYLTHIO) 4,9 DIHYDROFURO [3,4 B]QUINOLIN 1(3H)ONE; 9 (4 FLUOROPHENYL) 6 (METHYLTHIO) 4,9 DIHYDROFURO[3,4 B] QUINOLIN 1(3H)ONE; 9 (4 HYDROXY 3-METHOXYPHENYL) 5 (METHYLTHIO) 4,9 DIHYDROFURO[3,4 B]QUINOLIN 1(3H)ONE; 9 (4 METHOXYPHENYL) 6,9 DIHYDRO [1,3]DIOXOLO[4,5 G]FURO [3,4 B]QUINOLIN 8(5H)ONE; 9 (BENZO[D][1,3]DIOXOL 5 YL) 6 (DIFLUOROMETHOXY) 4,9 DIHYDROFURO[3,4 B]QUINOLIN 1(3H)ONE; 9 (BENZO[D][1,3]DIOXOL 5 YL) 6,9 DIHYDRO [1,3]DIOXOLO[4,5 G]FURO[3,4 B]QUINOLIN 8(5H)ONE; 9 (PERFLUOROPHENYL) 6,9 DIHYDRO [1,3]DIOXOLO[4,5 G]FURO[3,4 B]QUINOLIN 8(5H)ONE; ANTILEUKEMIC AGENT; ETOPOSIDE; PODOPHYLLOTOXIN DERIVATIVE; UNCLASSIFIED DRUG; UNINDEXED DRUG; ANTINEOPLASTIC AGENT; PODOPHYLLOTOXIN; TRYPAN BLUE;

ANTINEOPLASTIC ACTIVITY; ARTICLE; CELL VIABILITY ASSAY; CONTROLLED STUDY; DRUG POTENCY; DRUG SELECTIVITY; DRUG STRUCTURE; DRUG SYNTHESIS; EC50; HUMAN; HUMAN CELL; IC50; PHYSICAL CHEMISTRY; STRUCTURE ACTIVITY RELATION; ANALOGS AND DERIVATIVES; CELL PROLIFERATION; CELL SURVIVAL; CHEMICAL STRUCTURE; CHEMISTRY; DOSE RESPONSE; DRUG EFFECTS; DRUG SCREENING; HEK293 CELL LINE; LEUKEMIA; PATHOLOGY; SYNTHESIS; TUMOR CELL LINE;

ANTINEOPLASTIC AGENTS; CELL LINE, TUMOR; CELL PROLIFERATION; CELL SURVIVAL; DOSE-RESPONSE RELATIONSHIP, DRUG; DRUG SCREENING ASSAYS, ANTITUMOR; HEK293 CELLS; HUMANS; LEUKEMIA; MOLECULAR STRUCTURE; PODOPHYLLOTOXIN; STRUCTURE-ACTIVITY RELATIONSHIP; TRYPAN BLUE;

EID: 84946573781     PISSN: 02235234     EISSN: 17683254     Source Type: Journal    
DOI: 10.1016/j.ejmech.2015.10.009     Document Type: Article

References (65)

1. V.W. Rusch, D.J. Giroux, M.J. Kraut, J. Crowley, M. Hazuka, T. Winton, D.H. Johnson, L. Shulman, F. Shepherd, C. Deschamps, R.B. Livingston, D. Gandara, Induction chemoradiation and surgical resection for superior sulcus non-small-cell lung carcinomas: long-term results of southwest oncology group trial 9416, J. Clin. Oncol. 25 (2007) 313-318;
2. For a review on etoposide, see: K.R. Hande, Etoposide: four decades of development of a topoisomerase II inhibitor Eur. J. Cancer 34 (1998) 1514-1521.
3. A.D. Ho, T. Lipp, G. Ehninger, H.J. Illiger, P. Meyer, M. Freund, W. Hunstein, Combination of mitoxantrone and etoposide in refractory acute myelogenous leukemia-an active and well-tolerated regimen, J. Clin. Oncol. 6 (1988) 213-217;
4. D.W. Milligan, K. Wheatley, T. Littlewood, J.I.O. Craig, A.K. Burnett, Fludarabine and cytosine are less effective than standard ADE chemotherapy in high-risk acute myeloid leukemia, and addition of G-CSF and ATRA are not beneficial: results of the MRC AML-HR randomized trial, Blood 107 (2006) 4614-4622.
5. K.R. Hande, Clinical applications of anticancer drugs targeted to topoisomerase II, Biochim. Biophys. Acta 1400 (1998) 173-184;
6. E.L. Baldwin, N. Osheroff, Etoposide, topoisomerase II and cancer, Curr. Med. Chem. Anticancer Agents 5 (2005) 363-372.
7. Y. Hitotsuyanagi, M. Fukuyo, K. Tsuda, M. Kobayashi, A. Ozeki, H. Itokawa, K. Takeya, 4-aza-2,3-dehydro-4-deoxypodophyllotoxins: simple azapodophyllotoxin analogues possessing potent cytotoxicity, Bioorg. Med. Chem. Lett. 10 (2000) 315-317;
8. R. Labruère, B. Gautier, M. Testud, J. Seguin, C. Lenoir, S. Desbène-Finck, P. Helissey, C. Garbay, G.G. Chabot, M. Vidal, S. Giorgi-Renault, Design, synthesis, and biological evaluation of the first podophyllotoxin analogues as potential vascular-disrupting agents, Chem Med Chem. 5 (2010) 2016-2025;
9. A. Kamal, P. Suresh, A. Mallareddy, B.A. Kumar, P.V. Reddy, P. Raju, J.R. Tamboli, T.B. Shaik, N. Jain, S.V. Kalivendi, Synthesis of a new 4-aza-2,3-didehydropodophyllotoxin analogues as potent cytotoxic and antimitotic agents, Bioorg. Med. Chem. 19 (2011) 2349-2358;
10. F. Shi, X.-N. Zeng, G. Zhang, N. Ma, B. Jiang, S. Tu, Facile synthesis of new 4-aza-podophyllotoxin analogs via microwave-assisted multi-component reactions and evaluation of their cytotoxic activity, Bioorg. Med. Chem. Lett. 21 (2011) 7119-7123;
11. I.V. Magedov, L. Frolova, M. Manpadi, U.D. Bhoga, H. Tang, N.M. Evdokimov, O. George, G.K. Hadje, S. Renner, M. Getlic, T.L. Kinnibrugh, M.A. Fernandes, S.S. Van, W.F.A. Steelant, C.B. Shuster, S. Rogelj, O.W.A.L. van, A. Kornienko, Anticancer properties of an important drug lead podophyllotoxin can be efficiently mimicked by diverse heterocyclic scaffolds accessible via one-step synthesis, J. Med. Chem. 54 (2011) 4234-4246;
12. M.N. Semenova, A.S. Kiselyov, D.V. Tsyganov, L.D. Konyushkin, S.I. Firgang, R.V. Semenov, O.R. Malyshev, M.M. Raihstat, F. Fuchs, A. Stielow, M. Lantow, A.A. Philchenkov, M.P. Zavelevich, N.S. Zefirov, S.A. Kuznetsov, V.V. Semenov, Polyalkoxybenzenes from plants. 5. Parsley seed extract in synthesis of azapodophyllotoxins featuring strong tubulin destabilizing activity in the sea urchin embryo and cell culture assays, J. Med. Chem. 54 (2011) 7138-7149;
13. N.B. Chernysheva, D.V. Tsyganov, A.A. Philchenkov, M.P. Zavelevich, A.S. Kiselyov, R.V. Semenov, M.N. Semenova, V.V. Semenov, Synthesis and comparative evaluation of 4-oxa- and 4-aza-podophyllotoxins as antiproliferative microtubule destabilizing agents, Bioorg. Med. Chem. Lett. 22 (2012) 2590-2593;
14. A. Kamal, J.R. Tamboli, V.L. Nayak, S.F. Adil, M.V.P.S. Vishnuvardhan, S. Ramakrishna, Synthesis of a terphenyl substituted 4-aza-2,3-didehydropodophyllotoxin analogues as inhibitors of tubulin polymerization and apoptosis inducers, Bioorg. Med. Chem. 22 (2014) 2714-2723.
15. For a review on synthesis of APTs and biological evaluation, see: M.G. Botes, S.C. Pelly, M.A.L. Blackie, A. Kornienko, W.A.L. van Otterlo, Synthesis of 4-Azapodophyllotoxins with anticancer activity by multicomponent reactions Chem. Heterocycl. Compd. 50 (2014) 119-138.
16. A. Dömling, I. Ugi, Multicomponent reactions with isocyanides, Angew. Chem. Int. Ed. 39 (2000) 3168-3210;
17. J. Zhu, Recent developments in the isonitrile-based multicomponent synthesis of heterocycles, Eur. J. Org. Chem. (2003) 1133-1144;
18. D.J. Ramon, M. Yus, Asymmetric multicomponent reactions (AMCRs): the new frontier, Angew. Chem. Int. Ed. 44 (2005) 1602-1634;
19. D. Enders, C. Grondal, M.R.M. Huttl, Asymmetric organocatalytic domino reactions, Angew. Chem. Int. Ed. 46 (2007) 1570-1581;
20. B.B. Tourè, D.G. Hall, Natural product synthesis using multicomponent reaction strategies, Chem. Rev. 109 (2009) 4439-4486;
21. A. Dömling, W. Wang, K. Wang, Chemistry and biology of multicomponent reactions, Chem. Rev. 112 (2012) 3083-3135.
22. A. Dömling, Recent advances in isocyanide-based multicomponent chemistry, Curr. Opin. Chem. Biol. 6 (2002) 306-313;
23. J.J. Sahn, B.A. Granger, S.F. Martin, Evolution of a strategy for preparing bioactive small-molecules by sequential multicomponent assembly processes, cyclizations, and diversification, Org. Biomol. Chem. 12 (2014) 7659-7672;
24. T. Zarganes-Tzitzikas, A. Dömling, Modern multicomponent reactions for better drug syntheses, Org. Chem. Front. 1 (2014) 834-837.
25. Husson H.-P, Giorgi-Renault S., Tratrat C., Atassi G., Pierre A., Renard, P., Pfeiffer B. Dihydrofuro[3,4-b]quinolin-l-one compounds. French patent no. 99.14771, Nov 24, 1999. Extension no. 00403255.3, Nov 22, 2000;
26. C. Tratrat, S. Giorgi-Renault, H.-P. Husson, A multicomponent reaction for the one-pot synthesis of 4-aza-2,3-didehydropodophyllotoxin and derivatives, Org. Lett. 4 (2002) 3187-3189.
27. J. Frackenpohl, I. Adelt, H. Antonicek, C. Arnold, P. Behrmann, N. Blaha, J. Boehmer, O. Gutbrod, R. Hanke, S. Hohmann, H.M. Van, P. Loesel, O. Malsam, M. Melchers, V. Neufert, E. Peschel, U. Reckmann, T. Schenke, H.-P. Thiesen, R. Velten, K. Vogelsang, H.-C. Weiss, Insecticidal heterolignans-tubuline polymerization inhibitors with activity against chewing pests, Bioorg. Med. Chem. 17 (2009) 4160-4184.
28. S. Tu, Y. Zhang, J. Zhang, B. Jiang, R. Jia, J. Zhang, S. Ji, A simple procedure for the synthesis of 4-aza-podophyllotoxin derivatives in water under microwave irradiation conditions, Synlett (2006) 2785-2790;
29. R. Labruère, S. Desbène-Finck, P. Helissey, S. Giorgi-Renault, Design and effective synthesis of the first 4-aza-2, 3-didehydropodophyllotoxin rigid aminologue: a n-methyl-4-[(3, 4, 5-trimethoxyphenyl) amino) ]-1, 2-dihydroquinoline-lactone, J. Org. Chem. 73 (2008) 3642-3645;
30. N.G. Kozlov, S.L. Bondarev, A.P. Kadutskii, L.I. Basalaeva, F.S. Pashkovskii, Tetronic acid in reaction with aromatic aldehydes and 2-naphthylamine. Investigation of fluorescent and nonlinear-optical characteristics of compounds obtained, Russ. J. Org. Chem. 44 (2008) 1031-1037;
31. F. Shi, D. Zhou, S. Tu, Q. Shao, C. Li, L. Cao, An efficient microwave-assisted synthesis furo[3,4-b]-[4,7] phenanthroline and indeno[2,1-b][4,7]phenanthroline derivatives in water, J. Heterocycl. Chem. 45 (2008) 1065-1070;
32. D. Madec, F. Mingoia, G. Prestat, G. Poli, N-substituted tetronamides as ambident nucleophilic building blocks for the synthesis of new 4-aza-2, 3-didehydropodophyllotoxins, Synlett (2008) 1475-1478;
33. N.G. Kozlov, V.E. Agabekov, S.L. Bondarev, L.I. Basalayeva, A.P. Kadutskiu, Synthesis of carbonyl containing heterocyclic compounds and their fluorescent and nonlinear optical properties, Dokl. Nats. Akad. Nauk. Belarusi. 53 (2009) 64-67;
34. S. Tu, S. Wu, S. Yan, W. Hao, X. Zhang, X. Cao, Z. Han, B. Jiang, F. Shi, M. Xia, J. Zhou, Design and microwave-assisted synthesis of naphtho[2, 3-f] quinoline derivatives and their luminescent properties, J. Comb. Chem. 11 (2009) 239-242;
35. A. Kumar, A.E. Alegria, Synthesis of novel functionalized 4-Aza-2,3-didehydropodophyllotoxin derivatives with potential antitumor activity, J. Heterocycl. Chem. 47 (2010) 1275-1282;
36. C. Shi, J. Wang, H. Chen, D. Shi, Regioselective synthesis and in vitro anticancer activity of 4-aza-podophyllotoxin derivatives catalyzed by L-proline, J. Comb. Chem. 12 (2010) 430-434;
37. F. Shi, S. Zhang, S.-S. Wu, Y. Gao, S.-J. Tu, A diversity-oriented synthesis of pyrazolo[4,3-f]quinoline derivatives with potential bioactivities via microwave-assisted multi-component reactions, Mol. Divers. 15 (2011) 497-505;
38. J.-H. Peng, R.-H. Jia, N. Ma, G. Zhang, F.-Y. Wu, C. Cheng, S.-J. Tu, A facile and expeditious microwave-assisted synthesis of furo[3, 4-b] indeno[2, 1-f] quinolin-1-one derivatives via multicomponent reaction, J. Heterocycl. Chem. 50 (2013) 899-902;
39. A. Aillerie, V.L. De Talance, A. Moncomble, T. Bousquet, L. Pelinski, Enantioselective organocatalytic partial transfer hydrogenation of lactone-fused quinolones, Org. Lett. 16 (2014) 2982-2985;
40. N. Jeedimalla, J. Johns, S.P. Roche, Mechanistic investigation and implications of a sacrificial aniline for the tandem cascade synthesis of 4-aza-podophyllotoxin analogues, Tetrahedron Lett. 54 (2013) 5845-5848.
41. For full experimental details, description of the entire library of APTs 2 synthesis and biological evaluation, refer to the supporting information.
42. X. Cao, Y.T. Lee, M. Holmqvist, Y. Lin, Y. Ni, D. Mikhailov, H. Zhang, C. Hogan, L. Zhou, Q. Lu, M.E. Digan, L. Urban, G. Erdemli, Cardiac ion channel safety profiling on the ionworks quattro automated patch clamp system, Assay. Drug Dev. Techn. 8 (2010) 766-780;
43. R. Zang, D. Li, I.C. Tang, J. Wang, S.-T. Yang, Cell-based assays in highthroughput screening for drug discovery, Int. J. Biotechnol. Wellness Ind. 1 (2012) 31-51.
44. D.P. DiRocco, J. Bisi, P. Roberts, J. Strum, K.K. Wong, N. Sharpless, B.D. Humphreys, CDK4/6 inhibition induces epithelial cell cycle arrest and ameliorates acute kidney injury, Am. J. Physiol. Ren. Physiol. 306 (2014) F379-F388.
45. E.S. Sung, A. Kim, J.S. Park, J. Chung, M.H. Kwon, Y.S. Kim, Histone deacetylase inhibitors synergistically potentiate death receptor 4-mediated apoptotic cell death of human T-cell acute lymphoblastic leukemia cells, Apoptosis. 15 (2010) 1256-1269;
46. Q. Yao, B. Weigel, J. Kersey, Synergism between etoposide and 17-AAG in leukemia cells: critical roles for Hsp90, FLT3, topoisomerase II, Chk1, and Rad51, Clin. Cancer Res. 13 (2007) 1591-1600.
47. A. Kumar, V. Kumar, A.E. Alegria, S.V. Malhotra, N-hydroxyethyl-4-aza-didehydropodophyllotoxin derivatives as potential antitumor agents, Eur. J. Pharm. Sci. 44 (2011) 21-26.
48. N.A. Smith, J.A.W. Byl, S.L. Mercer, J.E. Deweese, N. Osheroff, Etoposide quinone is a covalent poison of human topoisomerase IIb, Biochemistry. 53 (2014) 3229-3236;
49. C. Hu, C.S. Lancaster, Z. Zuo, S. Hu, Z. Chen, J.E. Rubnitz, S.D. Baker, A. Sparreboom, Inhibition of OCTN2-mediated transport of carnitine by etoposide, Mol. Cancer Ther. 11 (2012) 921-929.
50. C.A. Lipinski, Drug-like properties and the causes of poor solubility and poor permeability, J. Pharmacol. Toxicol. Methods 44 (2000) 235-249;
51. C.A. Lipinski, F. Lombardo, B.W. Dominy, P.J. Feeney, Experimental and computational approaches to estimate solubility and permeability in drug discovery and development settings, Adv. Drug Deliv. Rev. 64 (2012) 4-17.
52. A.-E.F. Nassar, A.M. Kamel, C. Clarimont, Improving the decision-making process in the structural modification of drug candidates: enhancing metabolic stability, Drug Discov. Today 9 (2004) 1020-1028.
53. [a] P. Gaillard, P.-A. Carrupt, B. Testa, A. Boudon, Molecular lipophilicity potential, a tool in 3D QSAR: method and applications, J. Comput. Aided Mol. Des. 8 (1994) 83-96
54. C.A. Lipinski, F. Lombardo, B.W. Dominy, P.J. Feeney, Experimental and computational approaches to estimate solubility and permeability in drug discovery and development settings1, Adv. Drug Deliv. Rev. 46 (2001) 3-26
55. M. Congreve, R. Carr, C. Murray, H.A. Jhoti, 'Rule of three' for fragmentbased lead discovery? Drug Discov. Today 8 (2003) 876-877
56. M.M. Hann, G.M. Keserü, Finding the sweet spot: the role of nature and nurture in medicinal chemistry, Nat. Rev. Drug Discov. 11 (2012) 355-365.
57. D.F. Veber, S.R. Johnson, H.-Y. Cheng, B.R. Smith, K.W. Ward, K.D. Kopple, Molecular properties that influence the oral bioavailability of drug candidates, J. Med. Chem. 45 (2002) 2615-2623
58. J. Kelder, P.J. Grootenhuis, D. Bayada, L.C. Delbressine, J.-P. Ploemen, Polar molecular surface as a dominating determinant for oral absorption and brain penetration of drugs, Pharm. Res. 16 (1999) 1514-1519
59. K. Palm, K. Luthman, A.-L. Ungell, G. Strandlund, P. Artursson, Correlation of drug absorption with molecular surface properties, J. Pharm. Sci. 85 (1996) 32-39.
60. C. Abad-Zapatero, Ligand efficiency indices for effective drug discovery, Expert Opin. Drug Discov. 2 (2007) 469-488
61. C. Abad-Zapatero, E.J. Champness, M.D. Segall, Alternative variables in drug discovery: promises and challenges, Future Med. Chem. 6 (2014) 577-593.
62. E.P. Gillis, K.J. Eastman, M.D. Hill, D.J. Donnelly, N.A. Meanwell, Applications of fluorine in medicinal chemistry, J. Med. Chem. 58 (2015), http://dx.doi.org/10.1021/acs.jmedchem.5b00258 in press.
63. A.-E.F. Nassar, A.M. Kamel, C. Clarimont, Improving the decision-making process in the structural modification of drug candidates: enhancing metabolic stability, Drug Discov. Today 9 (2004) 1020-1028.
64. J.-H. Zhang, T.D.Y. Chung, K.R. Oldenburg, A simple statistical parameter for use in evaluation and validation of high throughput screening assays, J. Biomol. Screen 4 (1999) 67-73.
65. J. Inglese, D.S. Auld, A. Jadhav, R.L. Johnson, A. Simeonov, A. Yasgar, W. Zheng, C.P. Austin, Quantitative high-throughput screening: a titration-based approach that efficiently identifies biological activities in large chemical libraries, Proc. Natl. Acad. Sci. 103 (2006) 11473-11478.