DISTAMYCIN-A AND TALLIMUSTINE INHIBIT TBP BINDING AND BASAL IN-VITRO TRANSCRIPTION

被引：75

作者：

BELLORINI, M

MONCOLLIN, V

DINCALCI, M

MONGELLI, N

MANTOVANI, R

机构：

[1] UNIV MILAN,DIPARTIMENTO GENET & BIOL MICROORGANISMI,I-20133 MILAN,ITALY

[2] INST GENET & BIOL MOLEC & CELLULAIRE,F-67404 ILLKIRCH GRAFFENS,FRANCE

[3] IST RIC FARMACOL MARIO NEGRI,I-20157 MILAN,ITALY

[4] PHARMACIA FARMITALIA CARLO ERBA,NEVIANO RES CTR,I-20014 NEVIANO,ITALY

来源：

NUCLEIC ACIDS RESEARCH | 1995年 / 23卷 / 10期

关键词：

D O I：

10.1093/nar/23.10.1657

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The antibiotic distamycin A is a DNA minor groove binding drug (MGB) that recognizes a stretch of a least four ATs. The alkylating benzoyl mustard derivative tallimustine (FCE 24517) has powerfull anti-tumor activity. Using the electrophoretic mobility shift assay (EMSA) we determined that both compounds can prevent binding of TBP and, with 10-fold higher concentration, TBP-TFIIA (DA) and TBP-TFIIA-TFIIB (DAB) to a TATA box, Once formed, the DA and DAB complexes are more resistant to MGB challenge. Both drugs can inhibit basal in vitro transcription of a minimal TATA-containing promoter and similar concentrations are necessary for binding and transcriptional inhibition. Tallimustine shows strong selectivity by decreasing only correctly initiated transcripts. Even at high doses (20 mu M), however, they cannot disturb a competent pre-initiation complex or Pol II progression. This functional in vitro model will provide a way to investigate the activity of sequence-specific DNA binding drugs with potential anti-viral and anti-tumour activity and to develop novel more selective compounds.

引用

页码：1657 / 1663

页数：7

共 49 条

[1] SYNTHESIS, DNA-BINDING PROPERTIES, AND ANTITUMOR-ACTIVITY OF NOVEL DISTAMYCIN DERIVATIVES
ARCAMONE, FM
ANIMATI, F
BARBIERI, B
CONFIGLIACCHI, E
DALESSIO, R
GERONI, C
GIULIANI, FC
LAZZARI, E
MENOZZI, M
MONGELLI, N
PENCO, S
VERINI, MA
[J]. JOURNAL OF MEDICINAL CHEMISTRY, 1989, 32 (04) : 774 - 778
[2] BARBIERI B, 1989, P AM CANCER SOC, V29, P330
[3] BREATHNACH R, 1981, ANNU REV BIOCHEM, V50, P349, DOI 10.1146/annurev.bi.50.070181.002025
[4] DISTAMYCINS INHIBIT THE BINDING OF OTF-1 AND NFE-1 TRANSFACTORS TO THEIR CONSERVED DNA ELEMENTS
BROGGINI, M
PONTI, M
OTTOLENGHI, S
DINCALCI, M
MONGELLI, N
MANTOVANI, R
[J]. NUCLEIC ACIDS RESEARCH, 1989, 17 (03) : 1051 - 1059
[5] DNA SEQUENCE-SPECIFIC ADENINE ALKYLATION BY THE NOVEL ANTITUMOR DRUG TALLIMUSTINE (FCE-24517), A BENZOYL NITROGEN-MUSTARD DERIVATIVE OF DISTAMYCIN
BROGGINI, M
COLEY, HM
MONGELLI, N
PESENTI, E
WYATT, MD
HARTLEY, JA
DINCALCI, M
[J]. NUCLEIC ACIDS RESEARCH, 1995, 23 (01) : 81 - 87
[6] BROGGINI M, 1991, CANCER RES, V51, P199
[7] DIFFERENT TBP-ASSOCIATED FACTORS ARE REQUIRED FOR MEDIATING THE STIMULATION OF TRANSCRIPTION INVITRO BY THE ACIDIC TRANSACTIVATOR GAL-VP16 AND THE 2 NONACIDIC ACTIVATION FUNCTIONS OF THE ESTROGEN-RECEPTOR
BROU, C
WU, J
ALI, S
SCHEER, E
LANG, C
DAVIDSON, I
CHAMBON, P
TORA, L
[J]. NUCLEIC ACIDS RESEARCH, 1993, 21 (01) : 5 - 12
[8] WEIGHT MATRIX DESCRIPTIONS OF 4 EUKARYOTIC RNA POLYMERASE-II PROMOTER ELEMENTS DERIVED FROM 502 UNRELATED PROMOTER SEQUENCES
BUCHER, P
[J]. JOURNAL OF MOLECULAR BIOLOGY, 1990, 212 (04) : 563 - 578
[9] BURATOWSKI S, 1994, CELL, V77, P2
[10] Burton N, 1991, Protein Expr Purif, V2, P432, DOI 10.1016/1046-5928(91)90105-R

← 1 2 3 4 5 →