Quantitative High-Performance Liquid Chromatography−Electrospray Ionization Tandem Mass Spectrometry Analysis of Bis-<i>N</i>7-Guanine DNA−DNA Cross-Links in White Blood Cells of Cancer Patients Receiving Cyclophosphamide Therapy

Bhaskar, Matcha; Johnson, Lisa M.; Nie, Bei; Panchal, Dolly; Matter, Brock; Jacobson, Pamala A.; Tretyakova, Natalia

doi:10.1021/ac902923s

Cited by 34 publications

(52 citation statements)

References 24 publications

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“…18, 20, 49-52, 56, 59, 64 Recently, tandem mass spectrometry with stable isotope dilution has been employed to identify and quantitate some of these DNA adducts. 53, 54, 61-63 Collectively, the studies indicate that these electrophiles react predominantly at the N7 atom of dG, although N3-dA modification can also be significant. 66 The toxicity of mustard agents has been attributed to interstrand DNA cross-links.…”

Section: Discussionmentioning

confidence: 90%

“…One study reported the identification of bis-N7-guanine cross-links in white blood cells of cancer patients receiving cyclophosphamide therapy, 53 and sulfur mustard (bis-(2-chloroethyl)-sulfide, SM) also forms bis[2-(guanin-7-yl)ethyl]sulfide cross-links in tissues of rodents, and urine of rabbits exposed to SM. 62, 63 The potential formation of ring-opened FapyG adducts was not addressed in those studies.…”

Section: Discussionmentioning

confidence: 99%

“…The labile N7-G and N3-A nitrogen and sulfur mustard adducts and their cross-links are often thermally hydolyzed from DNA under neutral 8-10, 51, 57, 61 or acidic 9, 10, 24, 46, 48, 50, 52, 53, 59 conditions. Alternatively, enzymatic digestion to the nucleosides has also been employed.…”

Section: Discussionmentioning

confidence: 99%

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Characterization of Nitrogen Mustard Formamidopyrimidine Adduct Formation of Bis(2-chloroethyl)ethylamine with Calf Thymus DNA and a Human Mammary Cancer Cell Line

Gruppi

Hejazi

Christov

et al. 2015

Chem. Res. Toxicol.

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A robust, quantitative ultraperformance liquid chromatography ion trap multistage scanning mass spectrometric (UPLC/MS3) method was established to characterize and measure five deoxyguanosine (dG) adducts formed by reaction of the chemotherapeutic nitrogen mustard (NM) bis-(2-chloroethyl)ethylamine with calf thymus (CT) DNA. In addition to the known N7-guanine (NM-G) adduct and its crosslink (G-NM-G), the ring-opened formamidopyrimidine (FapyG) mono-adduct (NM-FapyG) and cross-links in which one (FapyG-NM-G) or both (FapyG-NM-FapyG) guanines underwent ring-opening to FapyG units were identified. Authentic standards of all adducts were synthesized and characterized by NMR and mass spectrometry. These adducts were quantified in CT DNA treated with NM (1 μM) as their deglycosylated bases. A two-stage neutral thermal hydrolysis was developed to mitigate the artifactual formation of ring-opened FapyG adducts involving hydrolysis of the cationic adduct at 37 °C, followed by hydrolysis of the FapyG adducts at 95 °C. The limit of quantification values ranged between 0.3 and 1.6 adducts per 107 DNA bases, when the equivalent of 5 μg DNA hydrolysate was assayed on column. The principal adduct formed was the G-NM-G cross-link, followed by the NM-G mono-adduct; the FapyG-NM-FapyG adduct was at the limit of detection. The NM-FapyG adducts formed in CT DNA at a level of ~20% that of the NM-G adduct. NM-FapyG has not been previously quanitified and the FapyG-NM-G and FapyG-NM-FapyG adducts have not be previously characterized. Our validated analytical method was then applied to measure DNA adduct formation in the MDA-MB-231 mammary tumor cell line exposed to NM (100 μM) for 24 h. The major adduct formed was NM-G (970 adducts per 107 bases), followed by G-NM-G (240 adducts per 107 bases) and NM-FapyG (180 adducts per 107 bases), and lastly the FapyG-NM-G cross-link adduct (6.0 adducts per 107 bases). These lesions are expected to contribute to the NM-mediated toxicity and genotoxicity in vivo.

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Section: Discussionmentioning

confidence: 90%

Section: Discussionmentioning

confidence: 99%

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Characterization of Nitrogen Mustard Formamidopyrimidine Adduct Formation of Bis(2-chloroethyl)ethylamine with Calf Thymus DNA and a Human Mammary Cancer Cell Line

Gruppi

Hejazi

Christov

et al. 2015

Chem. Res. Toxicol.

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“…Our data reveal that alkylating agents and bleomycin directly damage telomeres. Telomeres and the Terc gene may be at increased risk of the damage induced by alkylating agents, such as guanine DNA-DNA cross-links, because of their G-rich DNA sequences [39,40]. Although the target of bleomycin is still unclear, there is evidence that bleomycin treatment can induce DNA damage to the telomere region [15,36].…”

Section: Discussionmentioning

confidence: 99%

Effects of Four Chemotherapeutic Agents, Bleomycin, Etoposide, Cisplatin, and Cyclophosphamide, on DNA Damage and Telomeres in a Mouse Spermatogonial Cell Line1

Liu

Hales

Robaire

2014

Biology of Reproduction

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Treatment with chemotherapeutics agents may induce persistent DNA damage in male germ cells with the possibility of long-term consequences on fertility and progeny outcome. Telomeres, specialized structures at the physical ends of chromosomes, play an important role in the maintenance of genetic stability and in the response of somatic cells to anticancer drugs. Our objective was to test the hypothesis that exposure to bleomycin, etoposide, or cisplatin (the drugs used to treat testicular cancer) or cyclophosphamide (an anticancer agent and immunosuppressant) targets telomeres in the male germ line. C18-4 spermatogonial cells were exposed to bleomycin, etoposide, cisplatin, or 4-hydroperoxycyclophosphamide (4OOH-CPA, a preactivated analog of cyclophosphamide). All four anticancer drugs induced a significant increase in DNA damage in C18-4 cells, as assessed by gamma-H2AX immunofluorescence. Interestingly, the gamma-H2AX signal was localized to telomeres after treatment with bleomycin, cisplatin, and 4OOH-CPA, but not etoposide. Mean telomere lengths, the intensity of the telomere fluorescence in situ hybridization signal, telomerase activity, and the expression of the telomerase enzyme mRNA components, Tert and Terc, were reduced by exposure to cisplatin and 4OOH-CPA, but not by bleomycin or etoposide. Thus, although all four anticancer drugs induced DNA damage in this spermatogonial cell line, telomeres were not specifically affected by etoposide and only the two alkylating agents, cisplatin and 4OOH-CPA, induced telomere dysfunction. This telomere dysfunction may contribute to infertility and developmental defects in the offspring.

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“…Figure 5.18 shows the scores plot of live cells treated with an anticancer drug, cyclophosphamide monohydrate, and an untreated control group of cells. Cyclophosphamide monohydrate is an alkylating agent that acts on DNA at the seventh position of nitrogen in guanine bases [70][71][72] mutations [70][71][72][73][74]. It is a common chemotherapeutic in the treatment of various cancers [73,74].…”

Section: Scp Of Live Cells In Aqueous Environmentmentioning

confidence: 99%

Medical Applications of Infrared Spectral Imaging of Individual Cells

Diem

Schubert

Miljković

et al. 2014

Infrared and Raman Spectroscopic Imaging

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Quantitative High-Performance Liquid Chromatography−Electrospray Ionization Tandem Mass Spectrometry Analysis of Bis-N7-Guanine DNA−DNA Cross-Links in White Blood Cells of Cancer Patients Receiving Cyclophosphamide Therapy

Cited by 34 publications

References 24 publications

Characterization of Nitrogen Mustard Formamidopyrimidine Adduct Formation of Bis(2-chloroethyl)ethylamine with Calf Thymus DNA and a Human Mammary Cancer Cell Line

Characterization of Nitrogen Mustard Formamidopyrimidine Adduct Formation of Bis(2-chloroethyl)ethylamine with Calf Thymus DNA and a Human Mammary Cancer Cell Line

Effects of Four Chemotherapeutic Agents, Bleomycin, Etoposide, Cisplatin, and Cyclophosphamide, on DNA Damage and Telomeres in a Mouse Spermatogonial Cell Line1

Medical Applications of Infrared Spectral Imaging of Individual Cells

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