EP1919873A1 - Fredericamycin derivatives - Google Patents

Abstract

The invention relates to new fredericamycin derivatives, to pharmaceuticals comprising them or their salts, and to the use of the fredericamycin derivatives for treating disorders, especially tumoral disorders.

Description

 Fredericamycin DERIVATIVES

The invention relates to novel Fredericamycin derivatives, medicaments containing these or their salts, and the use of Fredericamycin derivatives for the treatment of diseases, in particular tumors.

Fredericamycin was isolated from Streptomyces griseus in 1981 and shows antitumor activity.

Fredericamycin and some Fredericamycin derivatives are known.

WO 2004/024696 describes an advantageous purification method of Fredericamycin.

In Heterocycles 37 (1994) 1893-1912, J. Am. Chem. Soc. 116 (1994) 9921-9926, J. Am. Chem. Soc. 116 (1994) 11275-11286, J. Am. Chem. Soc. 117 (1995) 11839-11849, JP 2000-072752 and J. Am. Chem. Soc. 123 (2001) various, also enantioselective, total syntheses of Fredericamycin A are described. In J. Am. Chem. Soc. 127 (2005) 16442-16452 describes the biosynthetic pathway of Fredericamycin A.

In US 4,673,768 alkali salts of Fredericamycin A are described. In US 4,584,377

Fredericamycin derivatives, especially on the ring A and B acylated derivatives described. In US 5,166,208 also Fredericamycin derivatives are described, in particular derivatives which carry on the ring A thio or amino substituents. The derivatives are produced semisythetically or completely synthetically. The derivatives are produced semisythetically or completely synthetically. In WO 03/080582 a variety of ferdericamycin derivatives are described, which are derivatized at the rings A, B, E and / or F. In WO 03/087060 further derivatives of Fredericamycin are disclosed, in particular those in which the ring E is further derivatized. In WO 2004/004713 further derivatives of rings A and B are disclosed. There is a great need to provide further Fredericamycinderivate, in particular, have changed impact profiles (side effects, etc.).

Surprisingly, it has been found that Fredericamycin derivatives, which are derivatized in particular on the ring A or on the rings A and E, are potent drugs. It has also been found a semisynthetic possibility to introduce residues on the ring A or on both rings A and E, which allow the effectiveness and, inter alia, to increase the water solubility of the derivatives. Further methods of derivatization known from the prior art can additionally be carried out on the derivatives according to the invention. An alternative has also been found to render water-soluble Fredericamycin derivatives in which cyclodextrin inclusion compounds are prepared.

The invention relates to novel Fredericamycin derivatives of general formula Ia or Ib:

each one

_R 1 is H, C 1 -C 6 -alkyl, cycloalkyl, C 1 -C ₄ -alkyl-cycloalkyl,

R2 is H, Ci-C ₄ alkyl, C ₂ -C ₁₄ -alkenyl, aryl, C ₁ -C ₄ alkyl-aryl _l heteroaryl, C _r C ₄ alkyl heteroaryl, C ₂ -C ₄ -alkenyl-heteroaryl , Cycloalkyl, C ₁ -C ₄ -alkyl-cycloalkyl, heterocycloalkyl, C ₁ -C ₄ -alkyl-heterocycloalkyl, C _m H ₂ m ₊ o- _p Yp (with m = 1 to 6, for o = 1, p = 1 to 2m + for m = 2 to 6, o = -1, p = 1 to 2m + o, for m = 4 to 6, o = -2, p = 1 to 2m + o, Y = independently selected from halogen, OH, OR21, _NH2, NHR21, NR21R22, SH, SR21), (CH _{2) r} CH ₂ NHCOR21, (CH _{2) r} CH ₂ OCOR21, (CH _{2) r} CH ₂ NHCSR21, (CH _{2) r} CH ₂ S (O) n R21 with n = 0,1, 2, (CH ₂ ) _r CH ₂ SCOR21, (CH ₂ ) _r CH ₂ OSO ₂ -R21, (CH ₂ ) _r CHO, CH ₂ -ON = CH-aryl, CH ₂ -ON = CH-hetaryl, CH ₂ -ON = CH-R21, CH ₂ -ON = CR21R22, CH ₂ -0-N = CH-cycloalkyl, = NS CH-aryl, CH = NS Hetaryl, (CH ₂ ) _r CH = NOH, (CH ₂ ) _r CH (OH) _R 21, - (CH ₂ ) _r CH = NOR 21, (CH ₂ ) _r CH = NOCOR 21, (CH ₂ ) _r CH = NOCH ₂ CONR21 R22, (CH _{2) r} CH = NOCH (CH ₃₎ CONR21 R22, - (CH _{2) r} CH = NOC (CH _{3) 2} CONR21 R22, (CH _{2) r} CH = N-NHCO-R23, (CH _{2) r} CH = N-NHC (O) NH-R23, (CH ₂ ) _r CH = N-NHC (S) NH-R23, (CH ₂ ) _r CH = N-NHC (NH) NH-R23, (CH ₂ ) _r CH = N-NHC (NH) -R23, (CH _{2) r} CH = N-NHCO-CH ₂ NHCOR21, (CH _{2) r} CH = NO CH ₂ NHCOR21, (CH _{2) r} CH = N-NHCS-R23, (CH _{2) r} CH = CR24R25 ( trans or ice), (CH ₂ ) _r COOH, (CH ₂ ) _r COOR21, (CH ₂ ) _r CONR 21 R22, - (CH ₂ ) _r CH = NR 21,

(CH ₂ ) _r CH = N-NR21 R22, , and the (CH ₂ ) _r - chain extended radical

(CH ₂ ) _r CH = NN- (C ₁ -C ₃ -alkyl-NX'R211R212R213R214) (with X '= NR215, O, S and R211, R212, R213, R214, R215 independently of one another H or C ₁ - C ₆ -alkyl), - (CH ₂ ) _r CH = N-NHSO ₂ -aryl, - (CH ₂ ) _r CH = N-NHSO ₂ -heteroaryl, where r = 0,1, 2,3,4,5 , preferably 0,

R21, R22 independently of one another C _r Ci ₄ alkyl, Ci-C ₁₄ ~ alkanoyl, C _r C ₆ alkylhydroxy, CRCE alkylamino, CRCE-alkylamino-Ci-Ce-alkyl, C _r C ₆ alkylamino-di-C _r C ₆ - alkyl, cycloalkyl, C ₁ -C ₄ alkyl-cycloalkyl, heterocycloalkyl, C _r C ₄ alkyl heterocycloalkyl, aryl, aryloyl, C ₁ -C ₄ -alkyl-aryl, heteroaryl, Heteroaryloyl, C ₁ -

C ₄ alkyl heteroaryl, cycloalkanoyl, C _r C ₄ alkanoyl-cycloalkyl, heterocycloalkanoyl, C _r C ₄ alkanoyl-heterocycloalkyl, C 1 -C ₄ alkanoyl-aryl, C _r C ₄ alkanoyl-heteroaryl, mono- and di-sugar residues which are linked via a carbon atom which would carry an OH group in the sugar, wherein the sugars are independently selected from the group consisting of

Glucuronic acid and its stereoisomers on all optical C atoms, aldopentoses, aldohexoses, including their deoxy compounds (such as glucose, deoxyglucose, ribose, deoxyribose),

R 23 independently of R 21, the same meanings as R 21 or CH ₂ pyridinium salts, CH ₂ -RI-CrCβ-alkylammonium salts,

R24 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, COOR21, CONR21 R22, NH _2, NHCOR21

R25 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, COOR21, CONR21R22, NH _2, NHCOR21

R24, R25 together are C ₄ -C 8 cycloalkyl,

R3 H, F, Cl, Br, I, OH, OR31, NO _2, NH _2, NHR31, NR31 R32, NHCHO,

NHCOR31, NHCOCF _3, CH _3-m hal _m (with Hal = Cl, F, particularly F, and m = 1, 2, 3), OCOR31, SCN, CN, N _3, CH ₂ NR331 R332 (with R331, R332 which independently of one another can assume the same meaning as R33), CH ₂ OH, CH ₂ OR33, CH ₂ SR33, C ₂ -C ₁₄ -alkyl, C ₂ -C ₁₄ -alkenyl, C ₂ -C ₁₄ -alkynyl, C ₂ -C ₁₄ -alkyl, C ₂ -C ₁₄ - alkenyl, C ₂ -C ₁₄ alkynyl, aryl, C _r C ₄ alkyl-aryl, heteroaryl, Ci-CVAlkyl-heteroaryl, wherein the aryl or Herteroaryle with another aryl, C _r C ₄ -Alky] -aryl, O aryl, C _r C ₄ -alkyl-O-aryl, heteroaryl, Ci-C ₄ alkyl heteroaryl, O-heteroaryl or C _r C ₄ alkyl-O-heteroaryl may be substituted, cycloalkyl, C _r C ₄ - Alkyl cycloalkyl, heterocycloalkyl, C _r C ₄ alkyl heterocycloalkyl, C _m H _{2m + 0} . _p Y _p (with m = 2 to 6, for o = 1, -1, p = 1 to 2m + o, for m = 4 to 6, o = -3, p = 1 to 2m + o, Y = independent from each other selected from the group halogen, OH, OR31, NH _2, NHR31, NR31R32, SH, SR31), CH ₂ NHCOR31, CH ₂ NHCSR31, CH ₂ S (O) NR31 with n = 0,1, 2, ₂ CH SCOR31,

CH ₂ OSO ₂ -R31, CHO, CH = NOH, CH (OH) R31, -CH = NOR31, -CH = NOCOR31, -CH = NOCH ₂ CONR31R32, -CH = NOCH (CH ₃₎ CONR31 R32, -CH = NOC (CH _{3) 2} CONR31 R32, -CH = N-NHCO-R33, -CH = N-NHCO-CH ₂ NHCOR31, -CH = NO-CH ₂ NHCOR31, -CH = N-NHCS-R33, -CH = CR34R35 (trans or ice), COOH, COOR31, CONR31R32,

-CH = NR31, -CH = N-NR31R32, (with X '=

NR315, O, S and R311, R312, R313, R314, R315 independently of one another are H or C _r C ₆ -alkyl), -CH = N-NHSO ₂ -aryl, -CH = N-NHSO ₂ -heteroaryl, and / or

SCN, CN, N _3, CH ₂ NR331R332 (with R331, R332, which can assume the same meaning as R33 independently of one another), _CH2 SR33,

R31, R32 independently of one another C _r C ₁₄ alkyl, Crd-rAlkanoyl, C _r C ₆ alkylhydroxy, C ₆ alkylamino, CRCE-alkylamino-Ci-Ce-alkyl, CRCE-alkylamino-di-CrCe-

Alkyl, cycloalkyl, C _r C ₄ alkyl-cycloalkyl, heterocycloalkyl, dC ₄ alkyl heterocycloalkyl, aryl, aryloyl, -C ₄ alkyl-aryl, heteroaryl, Heteroaryloyl, C ₁ - C ₄ alkyl-heteroaryl, cycloalkanoyl, C _r C ₄ alkanoyl-cycloalkyl, heterocycloalkanoyl, CrC ^ alkanoyl-heterocycloalkyl, Ci-C ₄ alkanoyl-aryl, CτC ₄ alkanoyl-heteroaryl, mono- and di-sugar residues which are linked via a carbon atom, which in the Sugar would carry an OH group, the sugars being independently selected from the group consisting of glucuronic acid and its stereoisomers on all optical C atoms, aldopentoses, aldohexoses including their deoxy compounds (such as glucose, deoxyglucose, ribose, deoxyribose),

R33 independently of R31, have the same meanings as R31 or CH ₂ pyridinium salts, CH ₂ tri-C ₁ -C ₆ -alkylammonmium salts, R34 independently of R31, the same meanings as R31 or H, CN, COCH ₃ ,

COOH, C00R21, CONR31 R32, NH _2, NHC0R31

R35 independently of R31, has the same meanings as R31, or H, CN, COCH _3, COOH, COOR31, CONR31R32, NH _2, NHC0R31

R 34, R 35 together form C ₄ -C ₈ -cycloalkyl,

R5 H, C ₁ -C ₆ -alkyl, cycloalkyl, C _r C ₄ alkyl-cycloalkyl, heterocycloalkyl, C ₁ -C ₄ - alkyl-heterocycloalkyl, aryl, C _r C ₄ alkyl-aryl, heteroaryl, C _r C _4- alkyl

heteroaryl,

R4, R6, R7 independently of one another are H, C ₁ -C ₆ -alkyl, CO-R41

R41 independent of R21, the same meanings as R21

X is O, S, NH, N-R8, where R8 can independently of R5 have the same meaning as R5 or R5 and R8 together with the N form a 4, 5, 6, 7 or 8-membered heterocycloalkyl ring, which may optionally be another heteroatom selected from the group N, O, S may contain

or X-R5 together equal to H, F, Cl, Br, I, N3

YF, Cl, Br, I ₁ N ₃ , CN, CH ₂ NRYI RY ₂ , CH ₂ OH, CH ₂ ORYI, CH ₂ SRYI, SCN, aryl, hetaryl (where RY1, RY2 are each independently the same as

R23 may have), NRY1RY2 together with the N form a 4, 5, 6, 7 or 8-membered heterocycloalkyl, which may optionally contain a further heteroatom selected from the group N, O, S, and together in X-R5 equal to F , Cl, Br, I, N3, Y can also be H, W-R51, with W = O, S, NH, N-R81, R81 and R51 independently the same

Meaning R5 and R81 together with the N form a 4, 5, 6, 7 or 8-membered heterocycloalkyl ring, which may optionally contain a further heteroatom selected from the group N, O, S, and / or H, W-R51, wherein W = O, S, NH, N-R81, wherein R81 and R51 independently may have the same meaning as R5 or R51 and R81 together with the N represents a 4, 5, 6, 7 or 8 membered heterocycloalkyl ring which may optionally contain a further heteroatom selected from the group N, O, S,

ZO, S, NR9, where R9 can be H or d-Ce-alkyl, means their stereoisomers, tautomers and their physiologically acceptable salts or inclusion compounds.

Preference is given to compounds of the formula IIa or IIb

wherein the meaning of the radicals R, X, Y and Z as stated above, their tautomers and their physiologically acceptable salts or inclusion compounds.

The invention further relates to compounds of the formula Ia, Ib, IIa or IIb in which the radicals R except R3, have the meanings given above and R3 to R3 equal to H at least doubled the water solubility while retaining all other radicals, preferably at least fivefold, more preferably at least tenfold, more preferably at least fiftyfold, especially fifteenfold, or even fivefoldfold. The increase in water solubility is e.g. on the introduction of groups that can form more hydrogen bonds and / or are polar and / or ionic. Preference is given to radicals R3 having increased water solubility and the meaning given in the formulas.

The invention also relates to compounds of the formula Ia, Ib, IIa or IIb in which the radicals R except R2 have the meanings given above and additionally R2 with respect to R 2 equal to CH =CH-CH =CH-CH _3, the water solubility, while retaining all other radicals, is at least doubled, preferably at least five times, more preferably at least ten times, particularly preferably at least fifty times, in particular one hundred times, or even fivefold. The increase in water solubility occurs, for example, through the introduction of groups that multiply

Can form hydrogen bonds and / or are polar and / or ionic. A key intermediate is compounds with an aldehyde function in R2. Preference is given to radicals R2 having increased water solubility and the meaning given in the formulas. Particularly preferred are derivatives with increased water solubility in R2 and R3.

Preferred radicals in _{R 2} are heteroaryl, cycloalkyl, C 1 -C ₄ -alkyl-cycloalkyl, heterocycloalkyl, C 1 -C ₄ -alkyl-heterocycloalkyl, C _m H _{2m +} O - _p Yp (where m = 1 to 6, for o = 1, p = 1 to 2m + o, for m = 2 to 6, o = -1, p = 1 to 2m + o, for m = 4 to 6, o = -2, p = 1 to 2m + o, Y = independent from each other selected from the group halogen, OH, OR21, NH _2, NHR21, NR21R22, SH, SR21), CH ₂ NHCOR21, CH ₂ NHCSR21, CH ₂ S (O) NR21 with n = 0,1,2, CH ₂ SCOR21, CH ₂ OSO ₂ -R21, CH (OH) R21, -CH = NOCOR21,

-CH = NOCH ₂ CONR21 R22, -CH = NOCH (CH ₃₎ CONR21 R22, -CH = NOC (CH _{3) 2} CONR21 R22, -CH = N-NHCO-R23, -CH = N-NHCO-CH ₂ NHCOR21 , -CH = NO-CH ₂ NHCOR 21, -CH = N-NHCS-R 23, -CH = CR 24 R 25 (trans or ice), CONR 21 R22, -CH = NR 21,

-CH = N-NR21R22, NR215, O, S and R211, R212,

R213, R214, R215 are independently H or d-Ce-alkyl), -CH = N-NHSO ₂ -aryl, - CH = N-NHS0 ₂ -heteroaryl,

Preference is furthermore given to compounds as indicated above, where the radicals R, preferably independently of one another, assume one or more of the following meanings:

_R 1 is H, C 1 -C ₅ -alkyl, cycloalkyl, in particular H,

R2 H ₁ C ₁ -C ₁₄ -A ^ yI _{1 is} C ₂ -C ₁₄ -alkenyl, aryl, C _r C ₄ alkyl-aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, C ₂ -C ₄ alkenyl Heteroaryl, cycloalkyl, C ₁ -

C ₄ alkyl-cycloalkyl, heterocycloalkyl, C _r C ₄ -alkyl-heterocycloalkyl, C _m H _{2m + 0-} pY _p (with m = 1 to 6, for o = 1, p = 1 to 2m + o; for m = 2 to 6, o = -1, p = 1 to 2m + o, for m = 4 to 6, o = -2, p = 1 to 2m + o, Y = independently selected from the group of halogen, OH , OR21, NH _2, NHR21, NR21 R22, SH, SR21), (CH _{2) r} CH ₂ NHCOR21, (CH _{2) r} CH ₂ OCOR21, (CH _{2) r} CH ₂ NHCSR21,

(CH ₂ ) _r CH ₂ S (O) n R 21 where n = 0.1, 2, (CH ₂ ) _r CH ₂ SCOR 21, (CH ₂ ) _r CH ₂ OSO ₂ -R 21, (CH ₂ ) _r CHO, CH ₂ -ON = CH-aryl, CH ₂ -ON = CH-hetaryl, CH ₂ -ON = CH-R 21, CH ₂ -ON = CR 21 R 22, CH ₂ -ON = CH-cycloalkyl, CH = NS-aryl, CH = NS hetaryl, (CH ₂ ) _r CH = NOH, (CH ₂ ) _r CH (OH) _R 21, - (CH ₂ ) _r CH = NOR 21, (CH ₂ ) _r CH = NOCOR 21, (CH ₂ ) _r CH = NOCH ₂ CONR21 R22 , (CH ₂ ) _r CH = NOCH (CH ₃ ) CONR 21 R 22, - (CH ₂ ) _r CH = NOC (CH ₃ ) ₂ CONR 21 R 22, (CH ₂ ) _r CH = N-NHCO-R 23, (CH ₂ ) _r CH = N-NHC (O) NH-R23, (CH ₂ ) _r CH = N-NHC (S) NH-R23, (CH ₂ ) _r CH = N-NHC (NH) NH-R23, (CH ₂ ) _r CH = N-NHC (NH) -R23, (CH ₂ ) _r CH = N-NHCO-CH ₂ NHCOR21, (CH ₂ ) _r CH = NO-CH ₂ NHCOR21, (CH ₂ ) _r CH = N- NHCS-R23, (CH _{2) r} CH = CR24R25 (trans or cis), _r COOH (CH ₂₎ (CH _{2) r} COOR21, (CH _{2) r} CONR21R22, - (CH _{2) r} CH = NR21,

(CH ₂ ) _r CH = N-NR 21 R 22, , and the (CH ₂ ) _r chain extended the rest

(CH ₂ ) _r CH = NN- (Ci-C ₃ alkyl-NX'R211R212R213R214) (with X ^; = NR215, O ₁ S and R211, R212, R213, R214, R215 independently H or C ₁ -C ₆ -

Alkyl), - (CH ₂ ) _r CH = N-NHSO ₂ -aryl,

- (CH ₂ ) _r CH = N-NHSO ₂ heteroaryl, with r = 0.1, 2,3,4,5, preferably 0, particularly preferred are C ₂ -C ₁₄ alkenyl, C _r C ₄ alkyl Heteroaryl, C ₂ -C ₄ -

Alkenyl heteroaryl, CH = NOH, CH = NOR21,

R21, R22 independently of one another -C ₆ alkyl, cycloalkyl, aryl, C _r C ₄ alkyl-aryl, heteroaryl, -C ₄ alkyl-heteroaryl

R 23 independently of R 21, the same meanings as R 21 or CH ₂ pyridinium salts, CH ₂ triCrC ₆ -alkylammonmium salts,

R24 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, COOR21, CONR21 R22, NH _2, NHCOR21

R25 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, COOR21, CONR21R22, NH _2, NHCOR21

R24.R25 together C ₄ -C ₈ ~ cycloalkyl,

R3 H, F, Cl, Br, I, OH, OR31, NO _2, NH _2, NHR31, NR31 R32, NHCHO, NHCOR31,

NHCOCF _3, CH _3-m hal _m (with Hal = Cl, F, particularly F, and m = 1, 2, 3), OCOR31, SCN, CN, N _3, CH ₂ NR331 R332 (with R331, R332, the independently of one another may have the same meaning as R33), CH ₂ OH, CH ₂ OR33, CH ₂ SR33, C ₂ -C ₁₄ -alkyl, C ₂ -C ₄ -alkenyl, C ₂ -C ₁₄ -alkynyl C ₂ -C ₁₄ alkyl, C ₂ -C ₁₄ alkenyl, C ₂ -C ₁₄ alkynyl, aryl, CrC ₄ alkyl aryl, heteroaryl, CrC ₄ alkyl heteroaryl, wherein the aryls or herteroaryls with another Aryl, C | -C ₄ -alkyl-aryl, O-aryl, C _r C ₄ -alkyl-O-aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, O-heteroaryl, or Ci-C ₄ -alkyl-O heteroaryl may be substituted, cycloalkyl, Ci-C ₄ alkyl-cycloalkyl, heterocycloalkyl, C _r C ₄ -alkyl heterocycloalkyl, C _m H _{2m + 0-p} Y _p (with m = 2 to 6, for o = 1 , -1, p = 1 to 2m + o; for m = 4 to 6, o = -3, p = 1 to 2m + o; Y = independently from each other selected from the group halogen, OH, OR31, NH _2, NHR31, NR31 R32, SR31 SH _1), CH ₂ NHCOR31, CH ₂ NHCSR31, CH ₂ S (O) NR31 with n = 0,1, 2, CH ₂ SCOR31, CH ₂ OSO ₂ -R31, CHO, CH = NOH , CH (OH) R31, -CH = NOR31, CH = ~ NOCOR31, -CH = NOCH ₂ CONR31 R32, -CH = NOCH (CH ₃₎ CONR31 R32, -CH = NOC (CH _{3) 2} CONR31R32, -CH = N-NHCO-R33,

-CH = N-NHCO-CH ₂ NHCOR31, -CH = NO-CH ₂ NHCOR31, -CH = N-NHCS-R33, -CH = CR34R35 (trans or ice), COOH, COOR31, CONR31 R32,

-CH = NR31, -CH = N-NR31 R32,

NR315, O, S and R311, R312, R313, R314, R315 independently of one another are H or C ₁ -C 6 -alkyl), -CH = N-NHSO ₂ -aryl,

-CH = N-NHSO ₂ -Heteroaryl, particularly preferably H, F, Cl, Br, I ₁ NR31 R32, in particular Br, I ₁ and / or

CH ₂ NR331 R332 (with R331, R332, which independently of one another can assume the same meaning as R33),

R331, R332 independently of one another C _r C ₄ alkyl,

R31, R32 independently of one another C _r C ₄ alkyl,

_R 5 is H, C ₁ -C ₃ -alkyl, cycloalkyl, heterocycloalkyl,

R4, R6, R7 independently of one another are H, C 1 -C ₅ -alkyl, CO-R41, in particular in each case H,

R41 independent of R21, the same meanings as R21

X is O, S, NH, N-R8, more preferably O, NH, N-Rδ, wherein R8 is the same

Meaning as R5 can assume and with N-R8 particularly prefers R5 and R8 form together with the N a 6-membered heterocycloalkyl ring, which may optionally contain another heteroatom selected from the group N, O and in particular piperazino or morpholino, is particularly preferred O, NH, or X-R5 together equal to H,

Y is H, F, Cl, Br, I, N ₃ , in particular Br, I

Z is O, S, NH, in particular O

means their stereoisomers, tautomers and their physiologically acceptable salts or inclusion compounds.

Further, it is preferable that if

R3 = SCN, CN, N _3, CH ₂ NR331R332 (with R331, R332, which can assume the same meaning as R33 independently of each other), CH ₂ SR33,

Y = H, W-R51, where W = O, S, NH, N-R81, where R81 and R51 independently of one another can assume the same meaning as R5 or R51 and R81 together with the N represents a 4, 5, 6, Form 7 or 8-membered heterocycloalkyl ring, which may optionally contain a further heteroatom selected from the group N, O, S, and if R 3 = H, F, Cl, Br, I,, OH, OR31, NO ₂ , NH ₂ , NHR31, NR31 R32, NHCHO, NHCOR31, NHCOCF _3, CH _3-m hal _m (with Hal = Cl ₁ F, particularly F, and m = 1, 2, 3), OCOR31, SCN, CN, N _3, CH ₂ NR331R332 (with R331, R332, which can independently of each other have the same meaning as R33),

CH ₂ OH, CH ₂ OR33, CH ₂ SR33, C ₂ -C ₁₄ -alkyl, C ₂ -C ₁₄ -alkenyl, C ₂ -C ₁₄ -alkynyl, C ₂ -C ₁₄ -alkyl, C ₂ -C ₁₄ - Alkenyl, C ₂ -C ₄ alkynyl, aryl, C _r C ₄ alkyl aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, where the aryls or herteroaryls with another aryl, Ci-C ₄ alkyl aryl , O-aryl, C _r C ₄ -alkyl-O-aryl, heteroaryl, C _r C ₄ alkyl-heteroaryl, O-heteroaryl or C _r C ₄ alkyl-O- heteroaryl may be substituted, cycloalkyl, -C ₄ - Alkyl-cycloalkyl, heterocycloalkyl, C ₁ -C ₄ -alkyl heterocycloalkyl, C _m H _{2m +} O -pY _P (with m = 2 to 6, for o = 1, -1, p = 1 to 2m + o; m = 4 to 6, o = -3, p = 1 to 2m + o; Y = independently of one another selected from the group halogen, OH, 0R31, NH _2, NHR31, NR31 R32, SH, SR31), CH ₂ NHCOR31 , CH ₂ NHCSR31, CH ₂ S (O) n R 31 with n = 0.1, 2, CH ₂ SCOR31, CH ₂ OSO ₂ -R31, CHO, CH = NOH, CH (OH) R 31, - CH = NOR31,

-CH = NOCOR31, -CH = NOCH ₂ CONR31 R32, -CH = NOCH (CH ₃₎ CONR31R32, -CH = NOC (CH _{3) 2} CONR31 R32, -CH = N-NHCO-R33, -CH = N-NHCO -CH ₂ NHCORSI ₁ -CH = NO-CH ₂ NHCORSI, -CH = N-NHCS-R33, -CH = CR34R35 (trans or ice), COOH, C00R31, C0NR31 R32,

-CH = NR31, -CH = N-NR31R32,

NR315, O ₁ S and R311, R312, R313, R314, R315 independently of one another H or C _r C ₆ alkyl), -CH = N-NHSO ₂ aryl, -CH = N-NHS0 ₂ -heteroaryl, Y = F, Cl, Br, I ₁ N ₃ , CN, CH ₂ NRYI RY ₂ , CH ₂ OH, CH ₂ ORYI ₁ CH ₂ SRYI, SCN, aryl, hetaryl (where RY1.RY2 are each independently the same meaning R23 may have), NRY1RY2 together with the N form a 4, 5, 6, 7 or 8-membered heterocycloalkyl, which may optionally contain a further heteroatom selected from the group N, O, S, and together in X-R5 equal to F ₁ Cl, Br, I ₁ N3, Y can also be H ₁ W-R51, with W = O, S, NH ₁ N-R81, R81 and R51 can independently assume the same meaning as R5 or R51 and R81 together with the N is a 4, 5, 6, 7 or 8-membered heterocycloalkyl ring, which may optionally contain a further heteroatom selected from the group N, O, S included.

Very particular preference is given to the compounds whose stereoisomers, tautomers and their physiologically tolerated salts or inclusion compounds selected from the group consisting of the compounds of the examples and the compounds which have combinations of the various substituents of the compounds of these examples.

Also preferred are medicaments containing the above compounds of formula I or II in addition to the usual carriers and excipients.

Preference is also given to the abovementioned medicaments in combination with other active ingredients for the treatment of tumors.

These compounds according to the invention are used for the preparation of medicaments for the treatment of tumors, in particular of those which can be treated by the inhibition of the topoisomerases I and / or II. Tumors which can be treated with the substances according to the invention are e.g. Leukemia, lung cancer, melanomas, prostate tumors and colon tumors. The compounds of the invention are also used for the preparation of medicaments for the treatment of tumors which can be treated by the inhibition of peptidyl prolyl isomerase PIN-1. Such tumors are especially prostate tumors and breast cancer.

Furthermore, the compounds according to the invention can be used for the preparation of medicaments for the treatment of atopic dermatitis, parasites and for immunosuppression.

In the description and the claims, the following definitions apply to the individual substituents:

The term "alkyl" by itself or as part of another substituent means a linear or branched alkyl chain radical of the length stated in each case and optionally a CH ₂ - may be replaced by a carbonyl group For example C _1-4 alkyl such as methyl. Ethyl, 1-propyl, 2-propyl, 2-methyl-2-propyl, 2-methyl-1-propyl, 1-butyl, 2-butyl, d. ₆ -alkyl [eg C _1-4 -alkyl, pentyl, 1-pentyl, 2-pentyl, 3-pentyl, 1-hexyl, 2-hexyl, 3-hexyl, 4-methyl-1-pentyl or 3,3- dimethyl-butyl.

The term "C 1 -C 6 -alkylhydroxy", by itself or as part of another substituent, means a linear or branched alkyl chain radical of the respectively indicated length, which may be saturated or unsaturated and carries an OH group, eg hydroxymethyl, hydroxyethyl, 1-hydroxypropyl, 2 hydroxypropyl.

The term "alkenyl" by itself or as part of another substituent means a linear or branched alkyl radical having one or more C = C double bonds of the respectively specified length, a plurality of double bonds are preferably conjugated. Thus, C _2-6 alkenyl eg ethenyl, 1-propenyl, 2-propenyl, 2-methyl-2-propenyl, 2-methyl-1-propenyl, 1-butenyl, 2-butenyl, 1, 3-butadienyl, 2,4-butadienyl, 1 Pentenyl, 2-pentenyl, 3-pentenyl, 1, 3-pentadienyl, 2,4-pentadienyl, 1, 4-pentadienyl, 1-hexenyl, 2-hexenyl, 1, 3-hexyl, 4-methyl-1-pentenyl or 3,3-dimethyl-butenyl.

The term "alkynyl" by itself or as part of another substituent means a linear or branched alkyl radical having one or more carbon-carbon triple bonds of the indicated for each length, where additional double bonds may be present. For example C _2-6 alkynyl such as ethynyl means , 1-propynyl, 2-propynyl, 2-methyl-2-propynyl, 2-methyl-1-propynyl, 1-butynyl, 2-butynyl, 1-pentynyl, 2-pentynyl, 3-pentynyl, 1, 4-pentadinyl , 1-pentyne-4-enyl, 1-hexynyl, 2-hexynyl, 1, 3-hexdiinyl, 4-methyl-1-pentynyl or 3,3-dimethylbutynyl.

The term "halogen" is fluorine, chlorine, bromine, iodine, preferably bromine and chlorine.

The term "NR21R22" or analogous NRx1Rx2 also stands for a dialkylamino group, wherein the two alkyl groups together with the N can also form a 5- or 6-membered ring.

The term "cycloalkyl", alone or as part of another substituent, includes saturated, cyclic hydrocarbon groups having from 3 to 8 carbon atoms, such as cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl, 4-methylcyclohexyl, cyclohexylmethylene, cycloheptyl or cyclooctyl.

The term "heterocycloalkyl" by itself or as part of another substituent includes cycloalkyl groups wherein up to two CH ₂ groups may be replaced by oxygen, sulfur or nitrogen atoms and another CH ₂ group may be replaced by a carbonyl function, eg pyrrolidine , Piperidine, morpholine or

The term "aryl" by itself or as part of another substituent includes aromatic ring systems having up to 3 rings in which at least one ring system is aromatic and having up to 3 substituents, preferably up to 1 substituent, wherein the substituents independently C ₁ -C ₆ -alkyl, OH, NO _2, CN, CF _3, 0R11, SH, SR11, d-Ce-alkyl hydroxy, C _r C ₆ alkyl-OR11, COOH, COOR11, CONH2, CONR 11 R 12, CHO, CH = NO-C _r C ₁₀ alkyl, C ₁ -C ₁₀ -AIk-I-enyl, NH _2, NHR 11, NR11R12, halogen can have, where the radicals R11, R12 independently of one another C _r C _1o alkyl, Cycloalkyl, C _r C ₄ alkyl cycloalkyl, mean.

Preferred aryls are next to phenyl and 1-naphthyl and 2-naphthyl:

The term "heteroaryl" by itself or as part of another substituent includes aromatic ring systems having up to 3 rings, and up to 3 identical or different heteroatoms N, S, O wherein at least 1 ring system is aromatic and containing up to 3 substituents, preferably up to 1 substituent, wherein the substituents independently of one another are C _r C ₆ alkyl, OH, NO _2, CN, CF _3, 0R11, SH, SR11, C ₁ -C ₆ - alkyl hydroxy, d-Cβ-alkyl ORH, COOH ₁ C00R11, CONH2, C0NR11 R12, CHO, CH = NO-C _r C ₁₀ alkyl, C ₁ -C ₁₀ alk-1-enyl, NH ₂ , NHR11, NR11R12, may have halogen, wherein the radicals _R 11, R 12 independently of one another can mean C ₁ -C ₁₀ -alkyl, cycloalkyl, C ₁ -C ₄ -alkyl-cycloalkyl.

Preferred heteroaryls are:

In particular, 2-furyl, 3-furyl, 2-thiophenyl, 3-thiophenyl, 3-pyridinyl, 4-pyridinyl, 4-isoxazolyl, 2-N-methylpyrrolyl, and 2-pyrazinyl are preferred. Very particularly preferred are these as radical R3.

The term "ring system" generally refers to 3, 4, 5, 6, 7, 8, 9, or 10 membered rings, preferred are 5 and 6 membered rings, further preferred are ring systems having one or two fused rings.

The compounds of the formula I can be present as such or, if they have acidic or basic groups, in the form of their salts with physiologically compatible bases or acids. Examples of such acids are: hydrochloric, citric, trifluoroacetic, tartaric, lactic, phosphoric, methanesulfonic, acetic, formic, maleic, fumaric, succinic, succinic, sulfuric, glutaric, aspartic, pyruvic, benzoic, glucuronic, oxalic, ascorbic and acetylglycine. Examples of bases are alkali metal ions, preferably Na, K, alkaline earth ions, preferably Ca, Mg, ammonium ions.

The compounds of the invention can be administered orally in the usual way. The application can also be carried out i.V., i.m., with vapors or sprays through the nasopharynx.

The dosage depends on the age, condition and weight of the patient and on the mode of administration. As a rule, the daily dose of active ingredient per person is between about 0.1 μg / kg and 1 g / kg when given orally. This dose may be given in 2 to 4 single doses or once a day as a slow-release form.

The new compounds can be used solid or liquid in the usual galenic application forms, for example as tablets, film-coated tablets, capsules, powders, granules, dragees, solutions or sprays. These are produced in the usual way. The active ingredients can be processed with the usual pharmaceutical aids such as tablet binders, fillers, preservatives, tablet disintegrants, flow regulators, plasticizers, wetting agents, dispersants, emulsifiers, solvents, retarding agents, antioxidants and / or propellants (see H. Sucker et al .: Pharmazeutische Technology, Thieme-Verlag, Stuttgart, 1978). The thus obtained Application forms normally contain the active ingredient in an amount of from 0.1 to 99% by weight.

Experimental part

Fredericamycin A is available by fermentation or totally synthetically by known methods. The Fredericamycinderivate according to the invention can be prepared either from Fredericamycin A or from known Federicamycinderivaten by specified methods directly or by variation of the methods given. The reduced forms of the formula I b and II b can be prepared by mild reducing agents from the corresponding compounds of formula I a and II a.

Production of substances

Fredericamycin (1) or Fredericamycin derivatives can be combined with halogenating agents such as N-chlorosuccinimide (NCS), bromosuccinimide (NBS), N-iodosuccinimide (NIS), fluorinating agents such as Selectfluor® or elemental Br ₂ , Cl ₂ , Interhalogenverbindungen in good yields to the corresponding Halogenated Fredericamycin derivatives are reacted (Scheme 1). Amination and subsequent second halogenation leads to bishalogenated Fredericamycin derivatives with different substitution patterns. (Scheme 2).

Schemes 1 and 2

Halogenation 1

Hall: F ₁ CI, Br, I

Hal2 independent of Hall: halogen

For the synthesis of further water-soluble fredericamycin derivatives, Fredericamycin (1) was first hydroxylated with osmium (IV) oxide on the diene side chain. (see scheme 3).

Scheme 3

Fredericamycin (1) (2)

a) OsO ₄ , N-methylmorpholine-N-oxide, CH ₂ Cl ₂₁ CH ₃ OH ₁ H ₂ O.

The Fredericamycin tetrol (2) also serves as an important intermediate for the synthesis of the Fredericamycin derivatives with increased solubility and / or profile of action mentioned in this patent. By iodate cleavage with sodium metaperiodate or carrier-bound periodate, the tetrol side chain can be degraded in very high yields to the Fredericamycin aldehyde (3) (see Scheme 4).

Scheme 4

a) NaIO ₄ -H ₂ O-DMF or supported-10 ₄ -H ₂ O-DMF

This aldehyde can be converted, for example, by brominating reagents such as N-bromosuccinimide, bromine or other bromine-generating reagents (or other Halogenierungsreagenzien) to the nuclear-brominated compound (4) or nuclear-halogenated compounds (see Scheme 5). Scheme 5

Fredericamycinaldehyd

As an example of a substance library, the aldehyde (3) e.g. be reacted with hydroxylamines and hydrazines to the corresponding R3 substituted oximes. Amine exchange, nucleophilic substitution or C-C linkages are shown in Scheme 6. Scheme 6

(3) Fredericamycinaldehyde

Nucleophilic substitution or C-C coupling

Nu: N3, CN, SCN, aryl, hetaryl In the following schemes, it will be shown on the basis of Fredericamycin and its derivatives how analogous derivatives of the invention can be obtained.

Electrophilic substitution on the E ring and replacement of the methoxy group on the A ring

1)

Fredericamycin and its Seitenkettensubstituiertzen derivatives can be with literature-known Dimethylrnethylen ammonium chloride (Mannich salt) under anhydrous

Conditions on the E ring Aminomethylieren.

The replacement of the methoxy moiety on the A-ring of Fredericamycins and the

Derivatives are possible through primary, secondary or aromatic amines. Here are the

Components with the corresponding primary or secondary amines at

Room temperature stirred in DMF or other inert solvent. For aromatic amines, a catalysis with Lewis acids such as tin (IV) chloride, etc. is required.

Halogenation with NBS or bromine yields the F ring halogenated derivatives (see scheme 7)

Scheme 7

R2. , R3

If the Mannich reaction is carried out with aqueous formaldehyde and amine on the desmethylated Fredericamycin, the aminomethylation takes place at the A ring. The OH function on the A ring can be converted via the triflate into the amino compound or alkoxy compound (see Scheme 8). Scheme 8

2)

Fredericamycin or Fredericamycin derivatives can be electrophilically substituted on the E ring with in situ produced dirhodane. (Scheme 9)

Scheme 9

Examples

example 1

(8S) -4 ', 9,9'-trihydroxy-5,7'-dibromo-6'-dimethylamino-1, 1', 3 ', 5', 8'-pentaoxo- 1, 1 '^ S' ^ '.ΘJ ^' - octahydrospiro [cyclopentafg] isoquinoline-8,2 ^'cyclopenta [b] naphthalenes] - 3-carbaldehyde (compound 1)

Brom dimethylamino Fredericamycin aldehyde 5.0mg (8.4μmol) are dissolved under N2 in 1ml dry dimethylformamide. At room temperature, 3.0 mg (16.9 μmol) of N-bromosuccinimide are added and stirred at room temperature. After 90 minutes is with

Diluted 15 ml of water and the precipitate sucked off. The residue, dried in vacuo, is taken up in 25 ml of dichloromethane, washed with water and, after drying, concentrated over sodium sulfate.

Yield: 3.5 mg (62% of theory) of red crystal powder: M / e = 673, λ _max = 507.0 nm.

Example 2

(8S) -4 ', ^9,9' trihydroxy-5,7'-dibromo-6'-dimethylamino-1,1 _'l 3', 5 ', 8'-pentaoxo-

1, r, 2,3 ^', 5', 6,7,8'-octahydrospiro [cyclopentafg] isoquinoline-8,2 ^'cyclopenta [b] naphthalenes] ~

3-carbaldehyde-O-isopropyl oxime (compound 2)

Bromodimethylamino Fredericamycinaldehyde-O-isopropyloxime 83.0 mg (128.0 μmol) are dissolved under N 2 in 2 ml of absolute dimethylformamide. At room temperature 128μl

0.1 M bromine solution in DMF was added. After 1 hour is added to 40ml of water.

The precipitated residue is filtered off with suction and then washed with methanol. After purification on Sephadex® LH-20 with dichloromethane / methanol / trifluoroacetic acid

30/20 / 0.1 gives 42.0 mg (45% of theory) of a red solid. M / e = 730.0; λ _max =

504. Onm

Example 3 (8S) -4 ', 9,9'-trihydroxy-5,7'-dibromo-6'-methylamino-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinolines-8,2'-cyclopenta [b] -naphthalenes] -1, 1 '-3', 5 ', 8 ^' (2H) -pentones (compound 3)

Methylamino Fredericamycin 53.8 mg (100 μmol) are dissolved under N 2 in 2 ml of absolute dimethylformamide. At room temperature, 200μl of 0.2M solution of N-

Bromosuccinimide added in DMF. After 16 hours, the solvent is in

Deducted high vacuum. The residue is over Sephadex® LH-20 with

Dichloromethane / methanol / trifluoroacetic acid 30/20 / 0.1 purified.

Yield: 52.0 mg (75% of theory) of red solid. M / e = 696.0; λ _max = 506.0nm.

Example 4 (8S) -4 ', 9,9'-trihydroxy-5,7'-dibromo-6'-morpholino-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [ g] isoquinoline-8,2 ^'cyclopenta [b] -naphtalene] -1, ^1' -3 ^{', 5',} 8 ^'(2H) - Pentone (compound 5)

Morpholino Fredericamycin 59.5 mg (100 μmol) are dissolved under N 2 in 2 ml of absolute dimethylformamide. At room temperature, 200 μl of 0.2M solution of N-bromosuccinimide in DMF are added. After 3 ^hours' are again 200 .mu.l of 0.2M NBS solution was added and further stirred for 1 hour. The solvent is removed in a high vacuum and the residue is purified on Sephadex® LH-20 with dichloromethane / methanol / trifluoroacetic acid 30/20 / 0.1. Repeat purification by preparative HPLC RP18 with acetonitrile / water. Yield: 23.0 mg (31% of theory) of red solid. M / e = 753.0; λ _max = 500.0nm.

Example 5 (8S) -4 ^{', 9,9'} trihydroxy-5,7 ^'-dibromo-6' -dimethylamino-1, 1 ^{', 3',} 5 ^{', 8'} ~ -pentaoxo

1, 1 ^{', 2,3',} 5 ^{', 6,7,8'} -octahydrospiro [cyclopenta [g] isoquinoline-8,2 ^'~ cyclopenta [b] naphthalenes] - 3-carbaldehyde-O-methyl oxime (Compound 9)

Brom dimethylamino Fredericamycin aldehyde-O-methyloxime 50.0 mg (80.3 μmol) are dissolved under N 2 in 5 ml of absolute dimethylformamide. At room temperature, 14.3 mg (80.3 μmol) of N-bromosuccinimide in 1 ml of DMF are added. After stirring for 3 hours at RT, the solvent is removed in a high vacuum and the residue is purified on Sephadex® LH-20 with dichloromethane / methanol / trifluoroacetic acid 80/10 / 0.1. Yield: 47.0 mg (83% of theory) of red solid. M / e = 702.0; λ _max = 504.0nm.

Example 6

(8S) -4 ', ^9.9' trihydroxy-5,7 ^{'-dibromo-6'-cyclopropylamino-3} - [(1E, 3E) -penta-1, 3-dienyl] -6,7-dihydrospiro [cyclopenta [ g] isoquinolines-8,2'-cyclopenta [b] -naphthalenes] -1, 1 ^' -3 ^' , 5 ^' , 8' (2H) -pentones (compound 10)

Cyclopropylamino Fredericamycin 56.5 mg (100.0 μmol) is dissolved under N 2 in 5 ml of absolute dimethylformamide. At room temperature, 36.0 mg (202.2 μmol) of N-bromosuccinimide dissolved in 2 ml of DMF are added. After stirring for 2 hours at RT, the solvent is removed in a high vacuum and the residue is purified on Sephadex® LH-20 with dichloromethane / methanol / trifluoroacetic acid 80/10 / 0.1.

Yield: 38.0 mg (52% of theory) of red solid. M / e = 723.0; λ _max = 504.0nm.

Example 7

(8S) -4 ', 9,9'-trihydroxy-5,7'-dibromo-6'-cyclopropylamino-1, r, 3', 5 ', 8'-pentaoxo-1, 1', 2, 3 ' , 5 ', 6,7,8'-octahydrospiro [cyclopenta [g] ^{isoquinoline-8,2'} cyclopenta [b] naphthalenes] - 3-carbaldehyde-O-methyl oxime (compound 12) Cyclopropylamino Fredericamycaldehyde methoxime 60.0 mg (108.0 μmol) are dissolved under N 2 in 5 ml of absolute dimethylformamide. At room temperature, 40.3 mg (226.8 μmol) of N-bromosuccinimide are added. After stirring for 2 hours at RT, the solvent is removed in a high vacuum and the residue is purified on Sephadex® LH-20 with dichloromethane / methanol / trifluoroacetic acid 80/10 / 0.1.

Yield: 28.0 mg (36% of theory) of red solid. M / e = 714.0; λ _max = 500.0nm.

Example 8

(8S) -4 ', 9,9'-trihydroxy-5,7'-dibromo-6'-cyclopropylamino-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [ g] isoquinolines-8,2'-cyclopenta [b] -naphthalenes] -1,1 ^' -3 ^' , 5 ^' , 8 ^' (2H) -pentones (compound 15)

2-Fluorethylamino bromo Fredericamycin 10.0 mg (15.4μmol) are dissolved under N 2 in 1 ml of absolute dimethylformamide. At room temperature 2.7mg (15.4μmol) of N-bromosuccinimide are added. Stir after 5 hours at RT is 100ml water / 1%

Added trifluoroacetic acid. The precipitate is filtered off with suction and washed with water. Yield: 4.0 mg (36% of theory) red solid. M / e = 729.0; λ _max = 504.0nm.

Example 9 (8S) -4 ^{', 9.9'} trihydroxy-7'-piperidinomethyl-6'-hydroxy-3 - [(1 E, 3E) -penta-1, 3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinoline-8,2 ^'cyclopenta [b] -naphtalene] -1, ^1' -3 ^{', 5',} 8 ^'(2H) - Pentone (compound 16)

Hydroxyfredericamycin (Desmethylfredericamycin) 20.0mg (38.1μmol) are placed under N2 in 4ml of ethanol. After the addition of 4.0μl (40.3μmol) piperidine and 3.2μl (

115.0 μmol) of 37% aqueous formaldehyde is stirred for 30 minutes at room temperature.

The mixture is then heated at reflux temperature for 3 hours. On 80ml of water (with 1%

Trifluoroacetic acid). Vacuum and dry in vacuo.

Yield: 23.0 mg (97% of theory) of red solid. M / e = 623.0; λ _max = 500.0nm.

Example 10

(8S) -4 ', ^9.9' trihydroxy-7'-dimethylaminomethyl-6'-hydroxy-3 - [(1E, 3E) -penta-1, 3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinolines-8,2'-cyclopenta [b] -naphthalenes] -1, 1 ^' -3 ^' , 5 ', 8 ^' (2H) -pentones (compound 18)

Hydroxyfredericamycin (desmethylfredericamycin) 200.0 mg (381.0 μmol) are placed under N 2 in 40 ml of ethanol. After the addition of 286.0μl (571.5μmol) of dimethylamine (2M in

Methanol) and 57.0μl (762.0μmol) of 37% aqueous formaldehyde is added for 30 minutes

Room temperature stirred. The mixture is then heated for 7 hours to 60 ⁰ C. Then it is added to 300 ml of cold water (with 1% trifluoroacetic acid). Vacuum and dry in vacuo.

Yield: 193.0 mg (87% of theory) of red solid. M / e = 583.0; λ _max = 504.0nm.

Example 11 1-Deoxy-5-C - [(8 R) -4] 9,9'-trihydroxy-6'-hydroxy-7'-dimethylamino-1, r, 3 ^' , 5 ^' , 8'-penta-oxo-1,1 ', 2,3', 5 ', 6,7,8'-octahydrospiro [cyclopenta [g] isoquinoline-8,2'-cyclopenta [b] - naphthalene] -3-yl] pentitol (Compound 20)

Hydroxyfredericamycin tetrol 22.5 mg (38.0 μmol) are placed under N 2 in 6 ml of ethanol. After the addition of 20.0μl (40.0μmol) of dimethylamine (2M in methanol) and 3.2μl (115.0μmol) of 37% aqueous formaldehyde is stirred for 30 minutes at room temperature. It is then heated for 26 hours at 60 ⁰ C. After cooling to 100 ml of water (with 1% trifluoroacetic acid). Vacuum and dry in vacuo. Yield: 21.0 mg (96% of theory) of red solid. M / e = 651.0; λ _max = 498.0nm.

Example 12

(δSJ) 'θ.g ^' -trihydroxy-SJ ^' -diiodo-e'-methylamino-S-KIE.SEJ-penta-I .S-dienyl-δ, Ⓒ dihydrospiro [cyclopenta [g] isoquinoline-8, 2'-cyclopenta [b] naphthalenes] -1, 1 '-3', 5 ', 8' (2H) -pentones (compound 24)

Methylamino Fredericamycin 50.0 mg (92.8μmol) are dissolved under N2 in 5 ml of absolute dimethylformamide. At room temperature, 48.8 mg (218.5 μmol) of N-iodosuccinimide are added. After stirring for 5 hours at RT, 100 ml of water / 1% trifluoroacetic acid are added. The precipitate is filtered off with suction and washed with water. Yield: 7.2 mg (10% of theory) of red solid. M / e = 791.0; λ _max = 506.0nm.

The compounds 4,6-8,11, 13,14,17,19,21-23,25-27 were prepared by analogous procedure.

The compounds have the following structures

Example 1a

(δSJ ^ '. ^θ.θ' trihydroxy-S-thiocyanato-e ^'methoxy-i .i'.S'.δ'.δ'-pentaoxo-i .i ^ .S '^' ey.. δ'-octahydrospiro [cyclopenta [g] isoquinoline-8,2'-cyclopenta [b] naphthalene] -3-carbaldehyde-0-methoxime (compound 1)

Fredericamycaldehyde methoxime 19.0 mg (35.8 μmol) is dissolved under N 2 in 2 ml of acetic acid. After adding 15.2mg (157.5μmol) of potassium rhodanide are at 50 ⁰ C 3.6μl (71.6μmol) of bromine dissolved in 1 ml of acetic acid was added. At 5O ⁰ C at intervals of 1h, 2h, 3.5h and 5h each of the above Kaliumrhodanid / bromine amount is added. After a total of 6 h, the reaction solution is added dropwise in 15OmI water. It is shaken twice with chloroform, dried over sodium sulfate and concentrated to dryness. Yield: 7.0 mg (33% of theory) of red crystal powder. M / e = 588, λ _max = 502.0nm.

Example 2a

(8S) -4 ^{', 9.9'} trihydroxy-5-thiocyanato-6'-methoxy-3 - [(1E, 3E) penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinoline -8,2'-cyclopenta [b] -naphthalenes] -1,1'-3 ', 5', 8 '(2H) -pentones (Compound 2)

Fredericamycin 20.0 mg (37.1 μmol) are dissolved under N 2 in 2 ml of acetic acid. After

7.9 mg (81.4 μmol) of potassium thiocyanate are added dropwise 1.9 μl (37.1 μmol) of bromine dissolved in 0.5 ml of acetic acid. After 3 hours, 39.5 mg (407.0 μmol) of potassium thiocyanate and 9.5 μl (185.5 μmoles) of bromine dissolved in 0.5 ml of acetic acid are added. The mixture is heated to 50.degree. After 3h the reaction mixture is added to 50 ml of water and the precipitate is filtered off with suction. Wash with water and dry. The residue is taken up in chloroform and shaken 4x with water. Dry and constrict.

Yield: 6.0 mg (27% of theory) of red crystal mass. M / e = 597, λ _max = 504.0nm.

The compounds 3a and 4a are prepared by analogous procedure.

Example 3a

(8S) -4 ', 9,9'-trihydroxy-6'-azido-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinoline-8,2 '-cyclopenta [b] -naphthalenes] -1, 1' -3 ', 5', 8 '(2H) -pentones (compound 5)

Hydroxyfredericamycin (desmethylfredericamycin) 10.0 mg (19.0 μmol) are dissolved under N 2 in 3 ml of dichloromethane. After addition of 3.2 .mu.l (19.0 .mu.mol) trifluoromethanesulfonic anhydride and 2.3 .mu.l (19.0 .mu.mol) of 2,6-lutidine at 0 ⁰ C is stirred for 10 minutes after. Allow to come to room temperature and add 1.3mg (19.0μmol)

Sodium azide added. Stir for 14 hours. The reaction solution is then diluted with 20 ml of dichloromethane / 1% trifluoroacetic acid. Shake 2x with water, the organic phase is dried over sodium sulfate and concentrated to dryness. The remaining residue is purified by preparative HPLC (RP18, acetonitrile / water / trifluoroacetic acid).

Yield: 8.0 mg (76% of theory) of red solid. M / e = 551.0; λ _max = 504.0nm.

Example 4a

(8S) -4 ', 9,9'-trihydroxy-5-dimethylaminomethyl-6'-methoxy-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinoline 8,2'-cyclopenta [b] naphthalenes] -1, 1 ^' -3 ^' , 5 ', 8 ^' (2H) -pentones (compound 6)

Fredericamycin 10.0mg (18.5μmol) are dissolved under N2 in 2ml absolute dimethylformamide. After the addition of 36.6 mg (391.0 μmol) of N.N-dimethylmethylenemammonium chloride in 1 ml of absolute dimethylformamide, the mixture is heated to 50.degree. After 24 hours the

Reaction solution in 70 ml of water / trifluoroacetic acid added. The aqueous phase is extracted 2x with dichloromethane. Dry over sodium sulfate and concentrate. The remaining residue is purified by preparative HPLC (RP18, acetonitrile / water / trifluoroacetic acid). Yield: 5.3 mg (48% of theory) of red solid. M / e = 597.0; λ _max = 504.0nm.

Example 5a

(8S) -4 ', 9,9'-trihydroxy-5-dimethylaminomethyl-6'-methylamine-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinolines-8,2'-cyclopenta [b] -naphthalenes] -1, 1 '-3', 5 ', 8' (2H) -pentones (compound 7)

5-Dimethylaminomethyl Fredericamycin (Compound 25) 10.0 mg (16.8 μmol) are dissolved under N 2 in 1.2 ml of absolute dimethylformamide. After the addition of 200.0μl (400.0μmol) Methylamine (2M in methanol). After 4 hours at 40 ⁰ C, the reaction solution is added to 60ml water / trifluoroacetic acid. The precipitate is filtered off with suction, washed with water and dried. The residue is purified by preparative HPLC (RP18, acetonitrile / water / trifluoroacetic acid). Yield: 4.2 mg (42% of theory) of red solid. M / e = 596.0; λ _max = 504.0nm.

Example 6a

(8S) -4 ', 9,9'-trihydroxy-5-dimethylaminomethyl-6'-morpholino-3 - [(1E, 3E) -penta-1,3-dienyl] -6,7-dihydrospiro [cyclopenta [g] isoquinoline -8,2'-cyclopenta [b] -naphthalenes] -1, 1 '-3 ^' , 5 ^' , 8 ^' (2H) -pentones (compound 8)

5-Dimethylaminomethyl Fredericamycin (Compound 25) 5.0 mg (8.4 μmol) is dissolved under N 2 in 0.5 ml of absolute morpholine. Stir for 1 hour at room temperature. The reaction solution is then added to 50 ml of water / trifluoroacetic acid. The precipitate is filtered off with suction, washed with water and dried.

Yield: 1.8 mg (33% of theory) of red solid. M / e = 652.0; λ _max = 504.0nm.

The compounds 3,4 were prepared according to the analogous procedure.

The compounds have the following structures:

Example A

Water Solubility of Fredericamycin Derivatives The water solubility of the various fredericamycin derivatives can be determined in 0.9% NaCI solution with a pH of 7.

Example B

Determination of the effectiveness of the compounds on the survival capacity of tumor cells (cytotoxic effect)

It will determine the effect of compounds on the survivability of human

Breast cancer cell line MCF7 measured. The cell line is determined at 37 ° C, 95% humidity and 5% CO2 in RPMI medium (Cambrex).

The cells are placed in a 96 well microtiter plate (Costar) with an initial density of 2400

Inoculated cells per well and cultured for 24 hours. The compounds are dissolved in DMSO, prediluted with cell medium and added to the wells. The cells are incubated for a further 48 hours with a concentration of the compounds between 2.4 nM and 10,000 nM at a volume of 50 μl.

To each well is added 50 μl cell titre GIo (Promega) and the microplate for 2

Incubated at room temperature on a shaker and then 10 minutes in the

Darkness left to stand. The luminescence is measured with a microplate reader and is proportional to the

Number of viable cells. The percentage inhibition of cell viability is calculated in comparison to (i) without cells and compound (100% inhibition) and (ii) with cells and without compound (no inhibition).

The concentration of the half-maximal inhibition (IC50) is determined with GraphPad Prism (GraphPad software), the controls corresponding to 0 and 100%. The structures and the effectiveness of the compounds according to the invention can be found in the following table:

Claims

claims

1. Compounds according to general formula Ia or Ib:

each one

_R 1 is H, C 1 -C 6 -alkyl, cycloalkyl, C 1 -C ₄ -alkyl-cycloalkyl,

R 2 is H, C ₁ -C ₁₄ -alkyl, C ₂ -C ₁₄ -alkenyl, aryl, C _r C ₄ alkyl-aryl, heteroaryl, C | -C ₄ alkyl heteroaryl, C ₂ -C ₄ alkenyl Heteroaryl, cycloalkyl, C ₁ -C ₄ -alkyl-cycloalkyl, heterocycloalkyl, C _m H _{2m + 0- p} Yp (with m = 1 to 6, for o = 1, p = 1 to 2m + o, for m = 2 to 6, o = -1, p = 1 to 2m + o; for m = 4 to 6, o = -2, p = 1 to 2m + o; Y = independently from each other selected from the group halogen, OH, OR21, NH _2, NHR21, NR21 R22, SR21 SH _1), (CH ₂ ) _r CH ₂ NHCOR21, (CH ₂ ) _r CH ₂ OCOR 21, (CH ₂ ) _r CH ₂ NHCSR 21, (CH ₂ ) _r CH ₂ S (O) n R 21 where n = 0,1, 2, (CH ₂ ) _r CH ₂ SCOR21, (CH ₂ ) _r CH ₂ OSO ₂ -R 2i, (CH ₂ ) _r CHO, CH ₂ -ON = CH-aryl, CH ₂ -ON = CH-hetaryl, CH ₂ -ON = CH-R 21 , CH ₂ -ON = CR 21 R 22, CH ₂ -ON = CH-cycloalkyl, CH = NS-aryl, CH = NS-hetaryl, (CH ₂ ) _r CH = NOH, (CH ₂ ) _r CH (OH) _R 21, - (CH ₂ ) _r CH = NOR 21, (CH ₂ ) _r CH = NOCOR 21, (CH ₂ ) _r CH = NOCH ₂ CONR 21 R 22, (CH _{2) r} CH = NOCH (CH ₃₎ CONR21 R22, - _(CH2) rCH = NOC (CH _{3) 2} CONR21 R22, (CH _{2) r} CH = N-NHCO-R23, (CH _{2) r} CH = N-NHC (O) NH-R23, (CH _{2) r} CH = N-NHC (S) NH-R23, (CH _{2) r} CH = N-NHC (NH) NH-R23, (CH _{2) r} CH = N-NHC (NH) -R 23, (CH _{2) r} CH = N-NHCO-CH ₂ NHCOR21, (CH _{2) r} CH = NO CH ₂ NHCOR21, (CH _{2) r} CH = N-NHCS- R23, (CH _{2) r} CH = CR24R25 (trans or cis), _r COOH (CH ₂₎ (CH _{2) r} COOR21, (CH _{2) r} CONR21 R22, - (CH _{2) r} CH = NR21,

(CH ₂ ) _r CH = N-NR 21 R 22, , and the (CH ₂ ) _r - chain extended radical

(CH ₂ ) rCH = NN- (C _r C 3 -alkyl-NX'R 2 11 R 212 R 213 R 214) (with X '= NR 215, O, S and R 2 11, R 2 12, R 2 13, R 2 14, R 215 independently of one another H or C ₁ -C ₆ -

Alkyl), - (CH ₂ ) _r CH = N-NHSO ₂ -aryl, - (CH ₂ ) _r CH = N-NHSO ₂ -heteroaryl, where r = 0,1,2,3,4,5, preferably 0 .

R21, R22 independently of one another C _r C ₁₄ alkyl, C _r C ₁₄ alkanoyl, CRCE-alkylhydroxy, CRCE-alkylamino, alkylamino-CRCE CRCE-alkyl, Ci-Ce-alkylamino-di-CrCe-

Alkyl, cycloalkyl, -C ₄ alkyl-cycloalkyl, heterocycloalkyl, C _r C ₄ alkyl heterocycloalkyl, aryl, aryloyl, C ₄ alkyl-aryl, heteroaryl, Heteroaryloyl, C ₁ - C ₄ alkyl-heteroaryl, cycloalkanoyl , -C ₄ alkanoyl cycloalkyl, heterocycloalkanoyl, CrGrAlkanoyl-heterocycloalkyl, C ₁ -C ₄ alkanoyl-aryl, C _r C ₄ alkanoyl-heteroaryl, mono- and di-sugar residues linked through a C atom which in the sugar would carry an OH group, wherein the sugars are independently selected from the group consisting of glucuronic acid and its stereoisomers of all optical carbon atoms, aldopentoses, aldohexoses including their deoxyverbidungen (such as glucose, deoxyglucose, ribose, deoxyribose),

R 23 independently of R 21, have the same meanings as R 21 or CH ₂ pyridinium salts, CH ₂ triC _r C ₆ alkylammonium salts,

R24 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, COOR21, CONR21 R22, NH _2, NHCOR21

R25 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, COOR21, CONR21R22, NH _2, NHCOR21

R24.R25 together are C ₄ -C 8 cycloalkyl,

R3 H, F, Cl, Br, I, OH, 0R31, NO _2, NH _2, NHR31, NR31 R32, NHCHO,

NHCOR31, NHCOCF _3, CH _{3. m} Hal _m (with HaI = Cl, F, in particular F, and m = Can take 1, 2, 3), OCOR31, SCN, CN, N _3, CH ₂ NR331R332 (with R331, R332 independently the same meaning as R33), CH ₂ OH, CH ₂ OR33, CH ₂ SR33, C C ₂ -C ₁₄ alkyl, C ₂ -C ₁₄ alkenyl, C ₂ -C ₁₄ alkynyl, C ₂ -C ₁₄ alkyl, C ₂ -C ₁₄ alkenyl, C ₂ -C ₁₄ alkynyl, aryl, C _r C ₄ alkyl aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, where the aryls or herteroaryls with another

Aryl, Ci-C ₄ -alkyl-aryl, O-aryl, C _r C ₄ -alkyl-O-aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, O-heteroaryl or C _r C alkyl _4-O- Heteroaryl may be substituted, cycloalkyl, C _r C ₄ alkyl cycloalkyl, heterocycloalkyl, C _r C ₄ alkyl heterocycloalkyl, C _m H _{2m + 0} . _p Y _p (with m = 2 to 6, for o = 1, -1, p = 1 to 2m + o, for m = 4 to 6, o = -3, p = 1 to 2m + o, Y = independent from each other selected from the group halogen, OH, OR31, NH _2, NHR31, NR31R32, SH, SR31), CH ₂ NHCOR31, CH ₂ NHCSR31, CH ₂ S (O) NR31 with n = 0,1, 2, ₂ CH SCOR31, CH ₂ OSO ₂ -R31, CHO, CH = NOH, CH (OH) R31, -CH = NOR31, -CH = NOCOR31, -CH = NOCH ₂ CONR31 R32, -CH = NOCH (CH ₃₎ CONR31R32, - CH = NOC (CH ₃ ) ₂ CONR31R32, -CH = N-NHCO-R33,

-CH = N-NHCO-CH ₂ NHCOR31, -CH = NO-CH ₂ NHCOR31, -CH = N-NHCS-R33, -CH = CR34R35 (trans or ice), COOH, COOR31, CONR31 R32,

-CH = NR31, -CH = N-NR31 R32, (with X '=

NR315, O, S and R311, R312, R313, R314, R315 independently of one another are H or C _r C ₆ -alkyl), -CH = N-NHSO ₂ -aryl,

-CH = N-NHSO ₂ heteroaryl, and / or

SCN, CN, N _3, CH ₂ NR331R332 (with R331, R332, which can assume the same meaning as R33 independently of one another), _CH2 SR33,

independently of one another C ₁ -C ₁₄ -alkyl, C _r C ₁₄ alkanoyl, C _r C ₆ alkylhydroxy, CRCE alkylamino, CRCE-alkylamino-d-Ce-alkyl, C _r C ₆ -Alkylannino-di ~ Ci-C ₆ - alkyl, cycloalkyl, C _r C ₄ alkyl-cycloalkyl, heterocycloalkyl, C _r C ₄ alkyl heterocycloalkyl, aryl, aryloyl, C _r C ₄ alkyl-aryl, heteroaryl, Heteroaryloyl, C ₁ - C ₄ alkyl Heteroaryl, cycloalkanoyl, CrC ^ alkanoyl-cycloalkyl,

Heterocycloalkanoyl, C _r C ₄ alkanoyl-heterocycloalkyl, C _r C ₄ alkanoyl-aryl, C _r C ₄ alkanoyl-heteroaryl, mono- and di-sugar residues which are linked via a carbon atom which in the sugar is an OH Group, wherein the sugars are independently selected from the group consisting of glucuronic acid and its stereoisomers on all optical carbon atoms,

Aldopentoses, aldohexoses including their deoxy compounds (such as glucose, deoxyglucose, ribose, deoxyribose), R33 independently of R31, have the same meanings as R31 or CH ₂ pyridinium salts, CH ₂ tri-C ₁ -C ₆ -alkylammonmium salts,

R34 independently of R31, has the same meanings as R31, or H, CN, COCH _3, COOH, COOR21, CONR31R32, NH _2, NHC0R31

R35 independently of R31, the same meanings as R31 or H, CN, COCH ₃ ,

COOH, C00R31, CONR31R32, NH _2, NHC0R31

R34.R35 together form C ₄ -C ₈ -cycloalkyl,

R5 is H, d-Cβ-alkyl, cycloalkyl, C _r C ₄ alkyl-cycloalkyl, heterocycloalkyl, C ₁ -C ₄ -

Alkyl-heterocycloalkyl, aryl, C ₁ -C ₄ -alkyl-aryl, heteroaryl, C ₁ -C ₄ -alkyl-heteroaryl,

R4, R6, R7 independently of one another are H, C _r C ₆ -alkyl, CO-R41

R41 independent of R21, the same meanings as R21

X is O, S, NH, N-R8, where R8 can independently of R5 have the same meaning as R5 or R5 and R8 together with the N form a 4, 5, 6, 7 or 8-membered heterocycloalkyl ring, which may optionally be another heteroatom selected from the group N, O, S may contain

or X-R5 together equal to H, F, Cl, Br, I, N3

YF, Cl, Br, I, N ₃ , CN, CH ₂ NRYI RY ₂ , CH ₂ OH, CH ₂ ORYI, CH ₂ SRYI, SCN, aryl,

Hetaryl (wherein RY1, RY2 may independently have the same meaning as R23), NRY1RY2 together with the N form a 4, 5, 6, 7 or 8 membered heterocycloalkyl ring, optionally one more

Heteroatom selected from the group N, O, S can contain, and in X-R5 together equal to F, Cl, Br, I, N3, Y can also be H, W-R51, with W = O, S, NH, N- R81, R81 and R51 independently of one another can assume the same meaning as R5 or R51 and R81 together with the N form a 4, 5, 6, 7 or 8-membered heterocycloalkyl ring which optionally contains a further heteroatom selected from the group consisting of N, O, S may contain, and / or

H, W-R51, wherein W = O, S, NH, N-R81, wherein R81 and R51 may independently be the same as R5 or R51 and R81 together with the N is 4, 5, 6, 7 or 8 membered

Form heterocycloalkyl ring, which may optionally contain a further heteroatom selected from the group N, O, S, Z is O, S, NR 9, where _R 9 can be H or C ₁ -C ₆ -alkyl,

means their stereoisomers, tautomers and their physiologically acceptable salts or inclusion compounds.

2. Compounds according to claim 1, wherein formula Ia or Ib, the stereochemistry of formula IIa or IIb

accepts.

3. Compounds of the general formula Ia, Ib, IIa or IIb according to claim 1 or 2, wherein the radicals R except R3, have the meanings given in the preceding claims and R3 to R3 equal to H, the water solubility while maintaining all other radicals at least doubled , preferably at least 5 times, more preferably at least 10 times, more preferably at least 50 times, in particular 100 times, or even 500 times.

4. Compounds of general formula Ia ₁ Ib, IIa or IIb according to claim 1 or 2, in which the radicals R except R2 have the meanings given in the preceding claims and R2 over R2 is CH = CH-CH = CH-CH ₃ the Water solubility while retaining all other radicals at least doubled, preferably at least five times, more preferably at least tenfold, particularly preferably at least fiftyfold, in particular one hundredfold, or even fivefoldfold.

5. Compounds according to any one of claims 1 to 4, wherein

R _{1 is} H, C ₁ -C ₅ -alkyl, cycloalkyl, in particular H,

R 2 is H, C ₁ -C ₁₄ -alkyl, C ₂ -C ₁₄ -alkenyl, aryl, C _r C ₄ alkyl-aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, C ₂ -C ₄ -alkenyl-heteroaryl , Cycloalkyl, C ₁ -

C ₄ alkyl cycloalkyl, heterocycloalkyl, C _r C ₄ alkyl heterocycloalkyl, C _m H _{2m +} O- _p Y _p (with m = 1 to 6, for o = 1, p = 1 to 2m + o; m = 2 to 6, o = -1, p = 1 to 2m + o, for m = 4 to 6, o = -2, p = 1 to 2m + o, Y = independently selected from the group halogen, OH, OR21, NH _2, NHR21, NR21 R22, SH, SR21), (CH _{2) r} CH ₂ NHCOR21, (CH _{2) r} CH ₂ OCOR21, (CH _{2) r} CH ₂ NHCSR21,

(CH ₂ ) _r CH ₂ S (O) n R 21 where n = 0.1, 2, (CH ₂ ) _r CH ₂ SCOR 21, (CH ₂ ) _r CH ₂ OSO ₂ -R 21, (CH ₂ ) _r CHO, CH ₂ -ON = CH-aryl, CH ₂ -ON = CH-hetaryl, CH ₂ -ON = CH-R 21, CH ₂ -ON = CR 21 R 22, CH ₂ -ON = CH-cycloalkyl, CH = NS-aryl, CH = NS-hetaryl, (CH ₂ ) _r CH = NOH, (CH ₂ ) _r CH (OH) _R 21, - (CH ₂ ) _r CH = NOR 21, (CH ₂ ) _r CH = NOCOR 21, (CH ₂ ) _r CH = NOCH ₂ CONR21 R22,

(CH _{2) r} CH = NOCH (CH ₃₎ CONR21 R22, - (CH _{2) r} CH = NOC (CH _{3) 2} CONR21 R22, (CH _{2) r} CH = N-NHCO-R23, (CH _{2) r} CH = N-NHC (O) NH-R23, (CH _{2) r} CH = N-NHC (S) NH-R23, (CH _{2) r} CH = N-NHC (NH) NH-R23, (CH _{2) r} CH = N-NHC (NH) -R23, (CH ₂ ) _r CH = N-NHCO-CH ₂ NHCOR21, (CH ₂ ) _r CH = NO-CH ₂ NHCOR21, (CH ₂ ) _r CH = N-NHCS -R23, (CH ₂ ) _r CH = CR 24 R 25 (trans or ice),

(CH _{2) r} COOH, (CH _{2) r} COOR21, (CH _{2) r} CONR21 R22, - (CH _{2) r} CH = NR21,

(CH ₂ ) _r CH = N-NR21 R22, , and the (CH ₂ ) _r chain-extended radical

_(CH2) rCH = NN (C ₁ -C ₃ alkyl-NX'R211 R212R213R214) (with X '= NR215, O, S, and R211, R212, R213, R214, R215 independently of one another H or C ₁ -C ₆ -

Alkyl), - (CH ₂ ) _r CH = N-NHSO ₂ -aryl,

- (CH ₂ ) _r CH = N-NHSO ₂ -Heteroaryl, with r = 0.1, 2,3,4,5, preferably O, particularly preferred are C ₂ -C ₁₄ alkenyl, C _r C ₄ alkyl -Het.eroaryl, C ₂ -C ₄ -

Alkenyl heteroaryl, CH = NOH, CH = NOR21,

_R 21, R 22 independently of one another are C ₁ -C ₆ -alkyl, cycloalkyl, aryl, C ₁ -C ₄ -alkyl-aryl, heteroaryl, C 1 -C ₄ -alkyl-heteroaryl R 23 independently of R 21, the same meanings as R 21 or CH ₂ pyridinium salts, CH ₂ tri-C ₁ -C ₆ -alkylammonmium salts,

R24 independently of R21, has the same meanings as R21, or H, CN, COCH _3, COOH, COOR21, CONR21R22, NH _2, NHCOR21

R25 independently of R21, the same meanings as R21 or H, CN, COCH ₃ ,

COOH, C00R21, CONR21R22, NH _2, NHC0R21

R24.R25 together form C ₄ -C ₈ -cycloalkyl,

R _{3 is} H, F, Cl, Br, I ₁ OH, OR31, NO ₂ , NH ₂ , NHR31, NR31 R32, NHCHO, NHC0R31,

NHCOCF _3, CH _{3-171 n} Hal (Hal = with Cl, F, particularly F, and m = 1, 2, 3), OCOR31, SCN, CN, N _3, CH ₂ NR331R332 (with R331, R332, the independently of one another can assume the same meaning as R33),

CH ₂ OH, CH ₂ OR33, CH ₂ SR33, C ₂ -C ₁₄ alkyl, C ₂ -C ₁₄ alkenyl, C ₂ -C ₁₄ alkynyl, C ₂ -C ₁₄ alkyl, C ₂ -C ₁₄ alkenyl , C ₂ -C ₄ alkynyl, aryl, C _r C ₄ alkyl aryl, heteroaryl, C ₁ -C ₄ alkyl heteroaryl, wherein the aryls or herteroaryls with another aryl, C _r C ₄ alkyl aryl , O-aryl, C _r C ₄ -alkyl-O-aryl, heteroaryl, C _r C ₄ alkyl heteroaryl, O-heteroaryl or C _r C ₄ alkyl-0-heteroaryl may be substituted, cycloalkyl, C _r C _4- alkyl-cycloalkyl, heterocycloalkyl, C ₁ -C ₄ -alkyl-heterocycloalkyl, C _m H _{2m + 0} .pY _p (with m = 2 to 6, for o = 1, -1, p = 1 to 2m + o, for m = 4 to 6, o = -3, p = 1 to 2m + o; Y = independently from each other selected from the group halogen, OH, 0R31, NH _2, NHR31, NR31R32, SH, SR31), CH ₂ NHCOR31, CH ₂ NHCSR31, CH ₂ S (O) n R31 with n = 0, 1, 2, CH ₂ SCOR31,

CH ₂ OSO ₂ -R31, CHO, CH = NOH, CH (0H) R31, -CH = NOR31, -CH = N0C0R31, -CH = NOCH ₂ CONR31 R32, -CH = NOCH (CH ₃₎ CONR31 R32, -CH = NOC (CH _{3) 2} CONR31 R32, -CH = N-NHCO-R33, -CH = N-NHCO-CH ₂ NHCORSI ₁ -CH = NO-CH ₂ NHCORSI, -CH = N-NHCS-R33, -CH = CR34R35 (trans or ice), COOH, COOR31, CONR31 R32,

-CH = NR31, -CH = N-NR31 R32, (with X '=

NR315, O, S, and R311, R312, R313, R314, R315 independently of one another H or C _r C ₆ alkyl), -CH = N-NHSO ₂ aryl, -CH = N-NHS0 ₂ -heteroaryl, particularly preferred are H, F, Cl, Br, I, NR31R32, in particular Br, I, and / or

CH ₂ NR331R332 (with R331, R332, which can independently of one another have the same meaning as R33), R331, R332 independently of one another C _r C ₄ alkyl,

R31, R32 independently of one another C ₁ -C ₄ -alkyl,

R 5 is H, C 1 -C ₃ -alkyl, cycloalkyl, heterocycloalkyl,

R 4, R 6, R 7 independently of one another are H, C 1 -C ₅ -alkyl, CO-R 4, in each case in each case H,

R41 independent of R21, the same meanings as R21

X is O, S, NH, N-R 8, more preferably O, NH, N-R 8, wherein R 8 is the same

Meaning as R5 can assume and with N-R8 particularly prefers R5 and R8 together with the N form a 6-membered heterocycloalkyl ring, which may optionally contain another heteroatom selected from the group N, O and in particular piperazino or morpholino, is particularly preferred O, NH,

or X-R5 together equal to H,

YH, F, Cl ₁ Br, I, N ₃ , in particular Br, I

Z is O, S, NH, in particular O

means.

6. Compounds according to any one of claims 1 to 5 in the form of inclusion compounds with cyclodextrin, in particular alpha-cyclodextrin.

7. Medicaments containing compounds according to any one of claims 1 to 6 in addition to the usual carriers and excipients.

8. Medicament according to claim 7 in combination with other active ingredients for tumor treatment.

9. Use of compounds according to any one of claims 1 to 6 for the preparation of medicaments for the treatment of tumors, in particular of those which can be treated by the inhibition of the topoisomerases I and / or II used.

10. Use of compounds according to any one of claims 1 to 6 for the preparation of medicaments for the treatment of parasites.

11. Use of compounds according to any one of claims 1 to 6 for the preparation of medicaments for immunosuppression.

12. Use of compounds according to any one of claims 1 to 6 for the preparation of medicaments for the treatment of atopic dermatitis.