Structural Characterization of Formaldehyde-Induced Cross-Links Between Amino Acids and Deoxynucleosides and Their Oligomers

Lü, Kun; Ye, Wenjie; Zhou, Li; Collins, Leonard B.; Chen, Xian; Gold, Avram; Ball, Louise M.; Swenberg, James A.

doi:10.1021/ja908282f

Cited by 161 publications

(146 citation statements)

References 27 publications

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“…In comparing the products of reactions containing lysine, cysteine, histidine, or tryptophan with each of the four DNA bases, the highest yield of crosslinked product was obtained with lysine and deoxyguanosine (51), consistent with lysine being the most reactive among residues in native proteins as described above. Similar results were obtained using short peptides and trinucleotides (51). In the context of protein-DNA interactions, the first chemical step could involve reaction with an amino acid side chain in a protein, the protein N terminus, or an amino or imino group on a DNA base; importantly, however, the ⑀-amino group on the lysine side chain is a better nucleophile than are the amino/imino groups on DNA bases whose lone pair electrons are delocalized in the aromatic ring.…”

Section: Capture Of Protein-dna Complexessupporting

confidence: 85%

Formaldehyde Crosslinking: A Tool for the Study of Chromatin Complexes

Hoffman

Frey

Smith

et al. 2015

Journal of Biological Chemistry

345

261

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Formaldehyde has been used for decades to probe macromolecular structure and function and to trap complexes, cells, and tissues for further analysis. Formaldehyde crosslinking is routinely employed for detection and quantification of protein-DNA interactions, interactions between chromatin proteins, and interactions between distal segments of the chromatin fiber. Despite widespread use and a rich biochemical literature, important aspects of formaldehyde behavior in cells have not been well described. Here, we highlight features of formaldehyde chemistry relevant to its use in analyses of chromatin complexes, focusing on how its properties may influence studies of chromatin structure and function.Prior to its use in the chromatin field, formaldehyde use had a long history in a number of fields, including vaccine production (1, 2) and histology (3). In this review, we focus on its use in chromatin immunoprecipitation approaches and protein-protein interaction studies applied to understand the location and abundance of transcription factor binding along DNA. A recent complementary perspective highlights gaps in knowledge with a particular focus on how formaldehyde crosslinking data have been used to interpret aspects of chromatin three-dimensional organization (4). Here, we briefly review prior work describing formaldehyde reactivity toward proteins, DNA, and their constituent monomers. This information provides a basis for understanding how formaldehyde functions in widely used assays in the chromatin field, and conversely, highlights less well understood aspects of formaldehyde behavior in cells. These issues are of significance for designing crosslinkingbased studies as well as for properly interpreting the resulting data. The analysis of formaldehyde-fixed chromatin has provided fundamental insights into where and when regulatory factors associate with the DNA template in vivo, but it in general does not provide unambiguous information about chromatin binding kinetics. A major goal of ongoing work is to understand kinetic and thermodynamic aspects of chromatin complex assembly at single copy loci in vivo. Development of experimental strategies to achieve these goals will require a deeper and more comprehensive understanding of the effects mediated by formaldehyde in cells.The following discussion provides a framework for understanding aspects of formaldehyde function when used to trap macromolecular complexes in cells, with the main features shown in Fig. 1. Beginning with basic chemical reactivity, this review will explore the ability of formaldehyde to crosslink with proteins and DNA to form protein-protein or protein-DNA complexes, common molecular quenchers, and the potential for crosslink reversal. Progress in capturing crosslinked complexes will also be discussed with an emphasis on the impact of a better understanding of formaldehyde chemistry in vivo. Basic ChemistryFormaldehyde is the smallest aldehyde, an electrophilic molecule susceptible to chemical attack by a wide range of nucleophilic species of ...

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Section: Capture Of Protein-dna Complexessupporting

confidence: 85%

Formaldehyde Crosslinking: A Tool for the Study of Chromatin Complexes

Hoffman

Frey

Smith

et al. 2015

Journal of Biological Chemistry

345

261

View full text Add to dashboard Cite

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“…Characterization and In Vitro Degradation of Formaldehyde-Induced DPCs Based on previous work in our lab (Lu et al, , 2010b, dG-Me-GSH and dG-Me-AGT are formed in vitro and contain specific dG-Me-Cysteine linkages (Fig. 1A).…”

Section: Resultsmentioning

confidence: 88%

“…Previous in vitro studies demonstrated DPCs were induced by formaldehyde with formation of N-CH 2 -N and N-CH 2 -S linkages between DNA and protein (Heck et al, 1990). To study the chemical identity of formaldehyde-induced DPCs, we investigated the in vitro crosslinking reaction between nucleosides, nucleotides, and amino acids and peptides in the presence of formaldehyde (Lu et al, 2010b). Our results demonstrate that the most abundant crosslink was formed with N-CH 2 -N linkage between dG and lysine.…”

Section: Discussionmentioning

confidence: 99%

“…However, it has not been possible to know the chemical identity of formaldehyde-induced DPCs formed in vivo due to the lack of chemical specific and accurate measurement. In this study, dG-Me-Cys containing N-CH 2 -S linkage was chosen for the degradation experiments based on its relatively high stability and abundance (Lu et al, 2010b). This study also included degradation of other crosslinks, dGMe-GSH, and dG-Me-AGT, both containing N-CH 2 -S linkage.…”

Section: Discussionmentioning

confidence: 99%

“…The synthesis of dG-Me-GSH was carried out according to a previous report (Lu et al, 2010b). Briefly, glutathione (85 mM) was incubated with formaldehyde (100 mM) in 1.75 ml sodium phosphate buffer (100 mM, pH 7.2) at 37 C for 4 h. dG was then added to a final concentration of 16 mM.…”

Section: Synthesis Of Dg-me-gsh Crosslinkmentioning

confidence: 99%

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Formation, Accumulation, and Hydrolysis of Endogenous and Exogenous Formaldehyde-Induced DNA Damage

Yu¹,

Lai²,

Hartwell³

et al. 2015

Toxicol. Sci.

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Formaldehyde is not only a widely used chemical with well-known carcinogenicity but is also a normal metabolite of living cells. It thus poses unique challenges for understanding risks associated with exposure. N 2-hydroxymethyl-dG (N 2 -HOMedG) is the main formaldehyde-induced DNA mono-adduct, which together with DNA-protein crosslinks (DPCs) and toxicityinduced cell proliferation, play important roles in a mutagenic mode of action for cancer. In this study, N 2 -HOMe-dG was shown to be an excellent biomarker for direct adduction of formaldehyde to DNA and the hydrolysis of DPCs. The use of inhaled [ 13 CD 2 ]-formaldehyde exposures of rats and primates coupled with ultrasensitive nano ultra performance liquid chromatography-tandem mass spectrometry permitted accurate determinations of endogenous and exogenous formaldehyde DNA damage. The results show that inhaled formaldehyde only reached rat and monkey noses, but not tissues distant to the site of initial contact. The amounts of exogenous adducts were remarkably lower than those of endogenous adducts in exposed nasal epithelium. Moreover, exogenous adducts accumulated in rat nasal epithelium over the 28-days exposure to reach steady-state concentrations, followed by elimination with a half-life (t 1/2 ) of 7.1 days. Additionally, we examined artifact formation during DNA preparation to ensure the accuracy of nonlabeled N 2 -HOMe-dG measurements. These novel findings provide critical new data for understanding major issues identified by the National Research Council Review of the 2010 Environmental Protection Agency's Draft Integrated Risk Information System Formaldehyde Risk Assessment. They support a data-driven need for reflection on whether risks have been overestimated for inhaled formaldehyde, whereas underappreciating endogenous formaldehyde as the primary source of exposure that results in bone marrow toxicity and leukemia in susceptible humans and rodents deficient in DNA repair.

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Engineered Smart Gating Nanochannels for High Performance in Formaldehyde Detection and Removal

Kai

Kong

Xiao

et al. 2019

Adv Funct Materials

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Bioinspired nanochannels for smart mass transport control have shown great potential for various applications in nanofluids, biosensing, and separation. Here, a nanochannel-based smart responsive platform exhibiting high formaldehyde (HCHO) sensitivity is designed and successfully fabricated by functionalizing the inner pore surface with ethylenediamine (EDA). By employing the nucleophilic addition reaction between HCHO and EDA immobilized on the nanochannels, the artificial nanochannels can switch from an open state to a closed state with the increase in HCHO. This is because the surface charge density and the wettability of the nanochannels change along with the HCHO immobilization. Meanwhile, the EDA-functionalized platform can hold a large amount of HCHO due to the abundant nanochannels of the membrane, so it presents a significant ability to remove HCHO in complex matrices. Also, the cultivation of mesenchymal stem cells in media containing HCHO can achieve excellent vitality in the presence of the EDA-functionalized nanochannels materials. This work paves an avenue for designing and developing bioinspired nanochannel based platform for harmful compounds detection and removal.

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Structural Characterization of Formaldehyde-Induced Cross-Links Between Amino Acids and Deoxynucleosides and Their Oligomers

Cited by 161 publications

References 27 publications

Formaldehyde Crosslinking: A Tool for the Study of Chromatin Complexes

Formaldehyde Crosslinking: A Tool for the Study of Chromatin Complexes

Formation, Accumulation, and Hydrolysis of Endogenous and Exogenous Formaldehyde-Induced DNA Damage

Engineered Smart Gating Nanochannels for High Performance in Formaldehyde Detection and Removal

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