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Published March 16, 2021 | Supplemental Material + Published
Journal Article Open

Role of intramolecular hydrogen bonds in promoting electron flow through amino acid and oligopeptide conjugates

Orłowski, Rafał ORCID icon
Clark, John A. ORCID icon
Derr, James B. ORCID icon
Espinoza, Eli M. ORCID icon
Mayther, Maximilian F. ORCID icon
Staszewska-Krajewska, Olga ORCID icon
Winkler, Jay R. ORCID icon
Jędrzejewska, Hanna ORCID icon
Szumna, Agnieszka ORCID icon
Gray, Harry B. ORCID icon
Vullev, Valentine I. ORCID icon
Gryko, Daniel T. ORCID icon

Abstract

Elucidating the factors that control charge transfer rates in relatively flexible conjugates is of importance for understanding energy flows in biology as well as assisting the design and construction of electronic devices. Here, we report ultrafast electron transfer (ET) and hole transfer (HT) between a corrole (Cor) donor linked to a perylene-diimide (PDI) acceptor by a tetrameric alanine (Ala)4. Selective photoexcitation of the donor and acceptor triggers subpicosecond and picosecond ET and HT. Replacement of the (Ala)4 linker with either a single alanine or phenylalanine does not substantially affect the ET and HT kinetics. We infer that electronic coupling in these reactions is not mediated by tetrapeptide backbone nor by direct donor–acceptor interactions. Employing a combination of NMR, circular dichroism, and computational studies, we show that intramolecular hydrogen bonding brings the donor and the acceptor into proximity in a "scorpion-shaped" molecular architecture, thereby accounting for the unusually high ET and HT rates. Photoinduced charge transfer relies on a (Cor)NH…O=C–NH…O=C(PDI) electronic-coupling pathway involving two pivotal hydrogen bonds and a central amide group as a mediator. Our work provides guidelines for construction of effective donor–acceptor assemblies linked by long flexible bridges as well as insights into structural motifs for mediating ET and HT in proteins.

Additional Information

© 2021 National Academy of Sciences. Published under the PNAS license. Contributed by Harry B. Gray, January 17, 2021 (sent for review December 28, 2020; reviewed by David N. Beratan and David I. Schuster). This work was supported by the National Science Centre, Poland (Grants HARMONIA 2016/22/M/ST5/00431 and PRELUDIUM 2016/23/N/ST5/00052), and the NSF (Grants CHE 1800602 and MPS AGEP-GRS to J.A.C.). A.S. and H.J. were supported by National Science Centre Grant 2017/25/B/ST5/01011 and Wroclaw Centre for Networking and Supercomputing Grant 299. Research at the California Institute of Technology was supported by the National Institute of Diabetes and Digestive and Kidney Diseases of the NIH under Award R01DK019038. The content is solely the responsibility of the authors and does not necessarily represent the official views of the NIH. Data Availability: All study data are included in the article and/or supporting information. R.O. and J.A.C. contributed equally to this work. Author contributions: R.O., V.I.V., and D.T.G. designed research; R.O., J.A.C., J.B.D., E.M.E., M.F.M., O.S.-K., and H.J. performed research; J.R.W., A.S., H.B.G., V.I.V., and D.T.G. analyzed data; and R.O., J.A.C., J.R.W., H.B.G., V.I.V., and D.T.G. wrote the paper. Reviewers: D.N.B., Duke University; and D.I.S., New York University. The authors declare no competing interest.

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Published - e2026462118.full.pdf

Supplemental Material - pnas.2026462118.sapp.pdf

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Additional details

Identifiers Funding Dates
Created:
August 22, 2023
Modified:
October 23, 2023