Anthracycline Antibiotics - American Chemical Society


Anthracycline Antibiotics - American Chemical Societyhttps://pubs.acs.org/doi/pdf/10.1021/bk-1995-0574.ch008intercalatin...

5 downloads 70 Views 621KB Size

Chapter 8 Synthesis of Anthraquinone Analogues of L i n k e d Anthracycline 1

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

Ping Ge and Richard A . Russell

2

1

2

Department of Medicinal Chemistry, State University of New York-Buffalo, Buffalo, NY 14260 School of Biological and Chemical Sciences, Deakin University, Geelong 3217, Australia

Molecules containing two anthraquinone moieties linked by an aliphatic chain and esterified by trans-4-aminocyclohexane carboxylic acid e.g. 34 have been prepared as simplified analogues oflinked anthracyclines e.g. 1. Although doxorubicin was discovered several decades ago the detailed mechanism of its action has proved elusive. While most anthracyclines are potential D N A intercalators, by nature of their planar quinonoidal chromophore, this property correlates only poorly with their antitumor activity. As a consequence, multimodal mechanisms^ have been advanced to account for the biological activity of this very significant group of chemotherapeutic agents. Recently, it has been suggested that D N A intercalators subvert the action of either or both of the DNA-regulatory isoenzymes topoisomerase Ha or l i b by stabilizing the enzyme-DNA complex (2,3). While little is known about the molecular details of this process, it has raised the possibility of designing drugs (4) that contain enhanced domains for both D N A and protein interaction. The isolation of the bis-intercalating quinoxalines such as Triostin A and Echinomycin, which span 2 bp (5), together with the related Luzopeptin, which appears to span 3 bp (6), has done much to keep alive the concept of D N A bisintercalating agents as potential therapeutic agents. Linked anthracyclines have also been the source of interest since the pioneering work of Henry and Tong (11) yielded the hydrazides 1. These compounds showed promising in vitro activity but they failed to trigger the promised rush of new clinical agents (12). Subsequent work by Reiss et al. added a range of anthracycline-based bisintercalators (13) which included the mixed acridine 2. While these compounds showed various degrees of promise, at least in vitro, much of the synthetic work was accomplished on a microscale and left unanswered the problem of how to produce larger quantities of these agents for further elaboration or modification (14). 0097-6156/95/0574-0132$08.00/0 © 1995 American Chemical Society

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

8. GE & RUSSELL

Anthraquinone Analogues of Linked Anthracycline H I

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

Ν

R I v

| f ^

R I

(CH^n ^

133

H I

γ

Ν

From a purely synthetic point of view, bis-intercalating anthracyclines have been largely ignored, no doubt in part because of the difficulties in attaching sugars efficiently to the latent aglycones. Despite many years of working with anthracyclines, we still find (15) that efficient glycosidation routes such as that described by Terashima (16,17) are sensitive to the nature of the aglycone and are frequently an experimental challenge. The prospect of developing totally synthetic routes to linked anthracyclines appeared limited until in the work of L i , Wang and Zhang (18,19,20) which suggested that the daunosaminyl group of doxorubicin or idarubicin could be replaced by an ester derived from trans 4-aminocyclohexane carboxylic acid 3, or by peptidyl variants 4 of this residue, and still leave high biological activity in the final molecule (13-14). At this point it seemed reasonable to pose the strategic problem as to how one might approach the synthesis oflinked anthracyclines. Should two completed units be joined in a penultimate step or should the two intercalators be constructed simultaneously from a linked precursor? The latter approach was clearly distinct from previous ones and offered possibilities for applying strategies based on the phthalide anion annelation of /?-quinone monoacetals (21-31) (Scheme I). This latter reaction has been an integral part of our endeavors in the anthracycline field and hence offered a good starting point.

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

134

ANTHRACYCLINE ANTIBIOTICS

9

10 Scheme I

The foundation work of Swenton's group (32,33) on the regioselective synthesis of pquinone monoacetals by anodic oxidation of 1,4-dimethoxybenzenes, followed by mild acid hydrolysis of the resulting bisacetals was readily applied to linked molecules (Scheme Π). Although the lack of total regioselectivity in the hydrolysis step lead to undesirable mixtures with hydrocarbon linking groups (11 L = CH2), the strategy provided an effective synthesis of polyether linked precursors (Scheme ΠΙ) and their subsequent annelated products (34). In this sequence the dienone 17 was formed in a 9:1 ratio with its regiomer, and could be isolated in a 51% yield. Conversion to the bis-anthrquinone was

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

Anthraquinone Analogues of Linked Anthracycline

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

8. GE & RUSSELL

Scheme m

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

135

136

ANTHRACYCLINE ANTIBIOTICS

achieved in 50% yield, a result considerably lower than yields achieved for simple quinone monoacetals. Similarly, some precursors containing secondary amide links e.g 19 were prepared in good yield and with a high regiospecificity controlled by the amide side chain (35).

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

(a) n = 2

(b) η = 4

Notwithstanding this success, the limited solubility in methanol of amides such as 20 severely limited the scale on which oxidations could be conducted. In addition the anodic oxidation of amides was frequently difficult and substrate dependent. Thus attempts to apply this approach to the N-methylated compound 22 (Scheme IV) failed completely and yielded only polymeric materials 23 (25).

A more satisfactory approach to the problem of regioselectivity lay in the observation that a variety of aryl ethers, (e.g.. TMS,TBDS, M O M and MEM)were labile towards anodic oxidation and could be converted to the corresponding dienone without the need for a hydrolysis step (Scheme V) (36).

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

8. GE & RUSSELL

Anthraquinone Analogues of Linked Anthracycline Ο

OR

© LiC10 /NaOAc MeOH 4

OMe

137

24

w M e

ù.

^ X °

R= IMS TBDS MOM MEM

M # O M e

25

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

Scheme V

Bearing in mind our earlier comments concerning the complexities of glycosidation, we were in the course of developing the aminocyclohexane carboxylate ester alternative when our rather limited bioassays revealed that the simple analogues (26 R=H or F) used as test vehicles for synthesis exhibited IC50 s in the range 0.02-0.04 m M in vitro against a P388 screen. Ο

OH

+

NH cr 3

These compared with levels of 0.001-0.002 m M for comparably substituted racemic daunomycins measured under identical conditions. This surprising activity for such simple molecules raised the prospect of adapting our chemistry to construct linked molecules containing the simpler anthraquinone nucleus. This was accomplished (Scheme VI) by reacting the aldehyde 27 with bisGrignard reagents (n=4,6,9) to afford 28 in average yields of 50%. Subsequent protection of the resulting alcohols (MOMCl/diisopropyl ethylamine, r.t.) afforded M O M ethers 29 in quantitative yield. Anodic oxidation of these substrates in anhydrous methanol containing lithium perchlorate and anhydrous sodium acetate afforded the bis /?-quinone monoacetals 30 which were efficiently annelated (65%) with cyanophthalide ion to afford the anthraquinones 31. Deprotection in two steps (H3O+, BCl3/-78°C) yielded 32 (86%) which was esterified by coupling with the protected (Moz) trans -4-aminocyclohexane carboxylic acid in the presence of D C C and D M A P , to yield ultimately the esters 33 (70%). Subsequent deprotection (HCl/dioxane) of the amides in 33 afforded the salts 34 (91%).These latter products were clearly a mixture of diastereomers as evidenced from their N M R spectra, and as such presumably contained isomers of varying activity .Accordingly the IC50 values in the range of 0.2-0.4 m M (P388 in vitro) provided only a crude measure of bioactivity and ignored synergistic or antagonistic effects.

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

138

ANTHRACYCLINE ANTIBIOTICS

or-

MOMO

M

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

M O>ΜΟ MO

e

Ο

I

2

°

MOMO

. Οη-\φ

7

-

^ ^ MOMO M OMO

I

MeOI

HO

ΟΜΟ

OMe I

ΟΜΟΜ ΟΜΟΜ

w

MeO

J***

OH

^ ^ . ΟOΜ MΟ OΜ M ^

w

w

Ο

M

w

ΟΜΟΜ 1

MeO^OMe

Y ""'"

""^X^

29 η = 4,6,9.

MeO^OMe

Ô

MOMO 30

Ο

OH

Ο

OMe

MeO

Ο

HO

Ο

ΟΜΟΜ

MOMO

O

Λ

Ο

OH

"9

OH

HO

OH

HO

NHMoz

Ο

OH

Ο

OH

«

Ο 32

Ο

Ο «

HO

Ο 33

Μ ο ζ Η Ν - ^ ^ " ^

0

\

^

ρ

Ο

ΜΌΖ = P - M E O P H C H O C O 2

ΟΗ

/^Γ™* ' Ο

ΗΟ

Ο

Η ΗΟ

Ο

OC^C^^^^ Ο

3*

ΟΗ

Ο Ο

*Η,Ν-

SchemeVI

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

8. GE & RUSSELL

Anthraquinone Analogues of Linked Anthracycline

139

Under the circumstances these initial results were not entirely discouraging. Nevertheless the low activities did not warrant the preparation of single optically pure stereoisomers. The fact that the hydrocarbon linking groups were far from optimal encouraged us to examine alternative strategies which could accommodate polyamide or polyamine linking chains. To this end we began to evaluate alternative synthetic routes which avoided anodic oxidation. Hypervalent iodine reagents e.g. PhI(OAc)2 emerged as alternative oxidants to generate p-quinone monoacetals under mild conditions (37,38). Our early findings suggest that there is a wealth of new chemistry which will provide easy access to precursors containing a variety of linking groups and at the same time these findings raise the prospect of incorporating minor groove binders such as distamycin (39-41) which may confer a better degree of site selectivity upon D N A intercalators. In the course of our investigations we found that the use of hypervalent iodine as an oxidant for phenols provides access to many o-quinone acetals 36 ( Scheme VII). The rapid nature of the oxidation coupled with the mild reaction conditions has enabled us to prepare and annelate a range of these molecules. While some oquinone monoacetals still dimerize too rapidly to be useful many survive long enough to act as Michael acceptors. This finding, has bestowed on phthalide anion annelation chemistry a new significance, and a range of alternatively substituted linked anthraquinones has begun to emerge. Q

PM(QAC)2



OMe

Φ5

fl

R , R = alkyl 1

cyanophthalide

V

35

2

Γ OMe

1' OH

Ψ

^OMe

Ri

37 Scheme VII

Acknowledgments We thank Mr. A . Mitchell for contributing some of his unpublished results to this paper. We also thank Professor R.N. Warrener, Central Queensland University, for his continuing interest and association with this work. Literature Cited 1. 2. 3.

Tritton, T.R.; Cell surface action of adriamycin. Pharmacol. and Ther. 1991, 49(3):291-309. Zunino, F.; Capraninco, G.; Anti-cancer Drug Design 1990, 5, 307-17. Tanako, H. Anticancer Drugs 1992, 3, 323-30.

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

140 4. 5. 6. 7.

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

8. 9. 10. 11. 12. 13. 14. 15. 16. 17. 18. 19. 20. 21. 22. 23. 24. 25. 26. 27. 28. 29. 30. 31. 32.

ANTHRACYCLINE ANTIBIOTICS Denny, W.A. Anticancer Drug Des. 1989, 4, 241-63. Low, C.M.L.; Drew, H.R.; Waring, M.J. Nucleic Acids Res. 1984, 12, 486579. Crothers,D.M.,Biopolymers 1968, 6, 575-84. Mikhailov, M.V.; Nikitin, S.M.; Zasedatelev, A.S.; Zhuze, A.L.; Guersky, G.V.; Gottikh, B.P. Febs. Lett. 1981, 136, 53-7. Acheson, R.M.; Constable,E.C.;Wright, R. McR.; Taylor, G.N. J. Chem. Res., (S) 1983, 2-3. Corey, M.; McKee, D.D.; Kagan, J.; Henry, D.W.; Millar, J.A. J. Am. Chem. Soc. 1985, 107, 2528-36. Gaugain, B.; Barbet, J.; Oberlin, R.; Roques,B.P.;Le PecqJ.B.Biochemistry 1978, 17, 5071-78. Henry, D.W.; Tong G.L.; U.S. Patent 4, 1978,112,217. Apple,M.A.;Yanagisawa, H.; Hut, C.A. Amer. Assoc. Cancer Res. Abstracts No. 675, 1978. Brownlee, R.T.C.; Cacoli, P.; Chandler, C.J.; Phillips,D.R.;Scourides, P.A.; Reiss, J.A. J. Chem. Soc., Chem. Commun. 1986, 659-61. Scourides, P.A.; Brownlee, R.T.C.; Phillips, D.R.; Reiss, J.A. J. Chromatogr. 1984, 288, 127-36. Russell, R.A.; Irvine, R.W.; McCormick, A.S.; Warrener, R.N. Tetrahedron 1988, 44, 4591-604. Kimura, Y.; Susuki, M.; Matsuomoto, T.; Abe, R.; Terashima, S. Chem. Lett. 1984, 502-4. Kimura, Y.; Susuki, M.; Matsumoto, T.; Abe, R.; Tershima, S. Bull. Chem. Soc. Japan 1986, 59, 423-31. Wang, Z.; Feng, D.; Zhang,C.;Acta Pharmaceutica Sinica 1984, 19 (5), 34956. Li, J.; Zhang, C.; Chinese Journal ofAntibiotics 1985, 10(4), 256-8. Li, J.; Zhang, C.; Pharmaceutical Industry 1986, 7(1), 15-20. Hauser, F.M.; Rhee, R.P. J. Am. Chem. Soc. 1977, 99 4533-34. Hauser, F.M.; Rhee, R.P. J. Org. Chem. 1978, 43, 178-80. Krauss, G.A.; Sugimoto, H. Tetrahedron Lett. 1978, 2263-66. Krauss, G.A.; Cho,H.;Crowley, S.; Roth, B.; Sugimoto,H.;Prugh, S. J. Org. Chem. 1983 48 3439-44. Russell, R.A.; Warrener, R.N. J. Chem. Soc., Chem. Commun. 1981, 108-10. Russell, R.A.; Pilley, B.A.; Irvine, R.W.; Warrener, R.N. Aust. J. Chem. 1987, Tatsuta, K.; Ozeki, H.; Yammaguchi, M.; Tanaka, M.; Okui, T. Tetrahedron Lett. 1990, 31, 5495-98. Dolson, M.G.; Chennard, B.L.; Swenton, J.S. J. Am. Chem. Soc. 1981, 103, 5263-64. Swenton, J.S.; Freskos, J.N.; Morrow, G.W.; Sercel, A.D. Tetrahedron 1984, 40, 4625-33. Keay, B.A.; Rodrigo, R. Can. J. Chem. 1985, 63, 735-38. Keay, Β.Α.; Rodrigo, R. Tetrahedron 1984, 40, 4597-607; Swenton, J.S. Acc. Chem. Res. 1983, 16, 74-81.

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.

8.

G E & RUSSELL

33. 34. 35.

Downloaded by UNIV OF CALIFORNIA SANTA BARBARA on May 9, 2016 | http://pubs.acs.org Publication Date: December 7, 1994 | doi: 10.1021/bk-1995-0574.ch008

36. 37. 38. 39. 40. 41.

Anthraquinone Analogues of Linked Anthracycline 141

Swenton, J.S. in The Chemistry of the Quinonoid Compounds; Patai, S.; Rappaport, Z. Ed.; John Wiley and Son, U.J., 1988, p. 899. Longmore, R.W.; Russell, R.A. Aust. J. Chem. 1991, 44, 1479-86. Russell, R.A.; Longmore, R.W.; Warrener, R.N. Aust. J. Chem. 1991, 44 1691-704. Russell, R.A.; Day, A.I.; Pilley, B.A.; Leavy, P.J.; Warrener, R.N. J. Chem. Soc., Chem. Commun. 1987, 1631-3. Fleck, A.E.; Hobart, S.A.; Morrow, G.W. Synth. Commun. 1992, 22, 179-87. Mitchell, A.I.; Russell, R. A. Tetrahedron Lett. 1993 545-48. Dervan, P.B.; Sluka, J.P. New Synthetic Methodology and Functionally Interesting Compounds; Elsevier NY 1986, pp. 307-322. Griffin, J.H.; Dervan, P.B. J. Am. Chem. Soc. 1987, 109, 6840-2. Wade, W.S.; Mrksich, M.; Dervan, P.B.; J. Am. Chem. Soc. 1992, 114, 878394.

RECEIVED August 3, 1994

Priebe; Anthracycline Antibiotics ACS Symposium Series; American Chemical Society: Washington, DC, 1994.