Infrared nanospectroscopic mapping of a single metaphase chromosome

Author:

Lipiec Ewelina123ORCID,Ruggeri Francesco S24ORCID,Benadiba Carine2,Borkowska Anna M1,Kobierski Jan D5ORCID,Miszczyk Justyna1,Wood Bayden R3,Deacon Glen B6,Kulik Andrzej2,Dietler Giovanni2,Kwiatek Wojciech M1

Affiliation:

1. Institute of Nuclear Physics, Polish Academy of Sciences, PL-31342 Krakow, Poland

2. Institute of Physics, Laboratory of Physics of Living Matter, Ecole Polytechnique Fédérale de Lausanne (EPFL), CH-1015 Lausanne, Switzerland

3. Centre for Biospectroscopy and School of Chemistry, Monash University, 3800 Victoria, Australia

4. Department of Chemistry, University of Cambridge, CB21EW, UK

5. Department of Pharmaceutical Biophysics, Faculty of Pharmacy Jagiellonian University Medical College, PL-31007 Cracow, Poland

6. School of Chemistry, Faculty of Science, Monash University, 3800 Victoria, Australia

Abstract

Abstract The integrity of the chromatin structure is essential to every process occurring within eukaryotic nuclei. However, there are no reliable tools to decipher the molecular composition of metaphase chromosomes. Here, we have applied infrared nanospectroscopy (AFM-IR) to demonstrate molecular difference between eu- and heterochromatin and generate infrared maps of single metaphase chromosomes revealing detailed information on their molecular composition, with nanometric lateral spatial resolution. AFM-IR coupled with principal component analysis has confirmed that chromosome areas containing euchromatin and heterochromatin are distinguishable based on differences in the degree of methylation. AFM-IR distribution of eu- and heterochromatin was compared to standard fluorescent staining. We demonstrate the ability of our methodology to locate spatially the presence of anticancer drug sites in metaphase chromosomes and cellular nuclei. We show that the anticancer 'rule breaker' platinum compound [Pt[N(p-HC6F4)CH2]2py2] preferentially binds to heterochromatin, forming localized discrete foci due to condensation of DNA interacting with the drug. Given the importance of DNA methylation in the development of nearly all types of cancer, there is potential for infrared nanospectroscopy to be used to detect gene expression/suppression sites in the whole genome and to become an early screening tool for malignancy.

Funder

National Science Center

Swiss National Science Foundation

Australian Research Council

Publisher

Oxford University Press (OUP)

Subject

Genetics

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