Marzia Bergomi scite author profile

Marzia Bergomi

5Publications

6Citation Statements Received

42Citation Statements Given

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Affiliations

Centro Ricerche FIAT, Fondazione IRCCS Istituto Nazionale dei Tumori

Publications

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Synthesis and Antitumor Activity of a New Class of Pyrazolo[4,3-e]pyrrolo[1,2-a][1,4]diazepinone Analogs of Pyrrolo[1,4][2,1-c]benzodiazepines

Baraldi¹,

Leoni²,

Cacciari³

et al. 1994

J. Med. Chem.

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A new class of pyrrolo[1,4]benzodiazepine (PBD) analogues featuring a pyrazolo[4,3-e]pyrrolo[1,2-a][1,4]diazepinone ring system has been designed and synthesized. These compounds, 2a-o, are characterized by the substitution of the aromatic A ring, characteristic of the PBDs, with a disubstituted pyrazole ring bearing alkyl and benzyl substituents at N6 or N7 and alkyl or carbomethoxy substituents at C8. Biological evaluation revealed an appreciable in vitro cytotoxic activity for compounds 2a,b,f-i.

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Eradication of a disseminated mouse lymphoma by 1,3‐BIS(2‐chloroethyl)‐1‐nitrosourea is immunologically mediated and accompanied by de novo generation of anti‐tumor cytotoxicity

Sensi

Bergomi

Formelli

et al. 1990

Intl Journal of Cancer

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The anti-tumor effect of 1,3-bis(2-chloroethyl)-1-nitrosourea (BCNU) was examined in BALB/c mice bearing increasing burdens of a syngeneic lymphoma (YC8). A single i.p. injection of the drug resulted in over 75% of cures when given at day 3, 5, 7 or 10 after an i.v. inoculum of 10(4) YC8 cells. The efficacy of BCNU on mice bearing large tumor burdens (from day 5 on) was not only due to its tumoricidal activity, but was immunologically mediated. Residual tumorigenic cells could be recovered in the livers of 5-day tumor bearers (TB) up to 2 weeks after BCNU treatment and only a low percentage of cures could be achieved when BCNU was administered to nude mice. In addition, BCNU-cured mice specifically rejected a lethal YC8 challenge and their splenocytes developed anti-tumor cytotoxicity in response to in vitro stimulation with YC8 cells. During kinetic experiments a 2-week period elapsed after BCNU injection before an anti-tumor cytotoxic T-lymphocyte (CTL) response could be generated by spleen cells of BCNU-treated 5-day TB. This period was characterized by immunosuppression as evaluated from impairment in the generation of lymphokine-activated killer (LAK) cells or of allospecific primary CTL responses by spleen cells from BCNU-treated 5-day TB and BCNU-treated normal mice. LAK cells first recovered and could be generated 7 days later, whereas primary allospecific CTL responses could only be detected by day 14, concomitantly with the generation of anti-tumor cytotoxicity by 5-day TB. The development of secondary in vitro CTL responses, however, was permanently abrogated. Spleen cells from BALB/c mice immunized either with YC8 or with DBA/2 minor histocompatibility antigens and treated with BCNU 1 week after the last immunization failed to mount an in vitro CTL response to their immunizing antigen, even when the cultures were supplemented with recombinant interleukin-2.

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Expression of retrovirus-related, cytotoxic T lymphocyte- and transplantation-defined antigens in NIH/3T3 transfectants after a single passage in nude mice.

Traversari

Carbone

Torre

et al. 1989

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Transfection of T24c-Ha-ras oncogene into NIH/3T3 fibroblasts resulted in the establishment of a transformed cell line (pT) that was tumorigenic when injected s.c. both into Swiss outbred nude mice and normal NIH inbred mice. The passage into nude mice, however, led to the development of a tumor variant (pT-nude) able to subsequently grow into sublethally x-irradiated but not into immunocompetent NIH mice. NIH mice immunized with this tumor variant developed a strong specific CTL response against the immunizing cell line, whereas the parental transformed pT cell line was not lysed. Clones were derived by limiting dilution from anti-pT-nude bulk population and were tested on a panel of transformed NIH/3T3 lines before and after their growth as tumor into nude mice. All of these lines were lysed by the Lyt-2+ CTL clones as a sole consequence of one in vivo passage into nude mice. The cross-reactive Ag were shown to be related to endogenous retroviral products as assessed by 1) immunoprecipitations of gp70, p15E, and p30 viral proteins in the nude variants but not in parental lines, and 2) by the ability of retroviruses from irradiated pT-nude cells to infect NIH/3T3 or pT lines making them susceptible to lysis by anti-pT-nude CTL clones. These results show that a single passage in nude mice can induce retrovirus-related, cell-surface Ag in transplanted neoplastic cells.

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Tricyclic indenopyridazine derivatives: Synthesis, cytotoxic activity and DNA‐binding properties

Barlocco¹,

Bergomi²,

Menta³

et al. 1996

Recl. Trav. Chim. Pays‐Bas

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Summary 2,4,4a,S-Tetrahydro-3 H-indeno [1,2-c]pyridazin-3-one (1)has been submitted to a series of modifications in order to obtain a new class of potential intercalating agents. In particular, insertion of a 4-4a double bond (2) and of a flexible cationic side-chain in the pyridazine moiety as well as introduction of substituents in several positions of the benzene ring have been considered. The dihydro analog 3 has been submitted to similar modifications. The new compounds have been tested for their cytotoxic activity on LoVo and LoVo/DX human colon carcinoma cell lines and on L1210 and L121O/CDPP murine leukemia cell lines, in comparison with cisplatin, melphalan and doxorubicin. Finally, to verify their intercalating properties, DNA-binding studies have been performed. Available evidence seems to indicate that the double bond in position 4-4a is essential for activity and that compounds derived from 2 are more potent than the corresponding compounds obtained from 3. Moreover, while a side-chain in position 2 led to active compounds, the 3-substituted indenopyridazines (8, 9) were inactive. The 2-[2-(dimethylamino)ethyl]2,5-dihydro-3H-indeno[ 1,2-c]pyridazin-3-one (5a) and its 8-methoxy derivative (5d) were found to compare favourably with cisplatin and melphalan, against resistant and both sensitive and resistant cell lines, respectively.

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ChemInform Abstract: Tricyclic Indenopyridazine Derivatives: Synthesis, Cytotoxic Activity and DNA‐Binding Properties.

Barlocco¹,

Bergomi²,

Menta³

et al. 1996

ChemInform

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Marzia Bergomi

Synthesis and Antitumor Activity of a New Class of Pyrazolo[4,3-e]pyrrolo[1,2-a][1,4]diazepinone Analogs of Pyrrolo[1,4][2,1-c]benzodiazepines

Eradication of a disseminated mouse lymphoma by 1,3‐BIS(2‐chloroethyl)‐1‐nitrosourea is immunologically mediated and accompanied by de novo generation of anti‐tumor cytotoxicity

Expression of retrovirus-related, cytotoxic T lymphocyte- and transplantation-defined antigens in NIH/3T3 transfectants after a single passage in nude mice.

Tricyclic indenopyridazine derivatives: Synthesis, cytotoxic activity and DNA‐binding properties

ChemInform Abstract: Tricyclic Indenopyridazine Derivatives: Synthesis, Cytotoxic Activity and DNA‐Binding Properties.

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