Multiple‐ion Management of Perovskites by Regulating Spatial Distribution of Hydroxyls in Oligosaccharides

Author:

Liu Xiaotao12,Jiang Xiaoqing2,Zhang Jiafeng23,Li Can2,Guo Xin2ORCID

Affiliation:

1. School of Materials Science and Engineering & National Institute for Advanced Materials Nankai University Tongyan Road 38 Tianjin 300350 China

2. State Key Laboratory of Catalysis Dalian Institute of Chemical Physics Chinese Academy of Sciences Dalian National Laboratory for Clean Energy Dalian 116023 China

3. University of Chinese Academy of Sciences Beijing 100049 China

Abstract

AbstractSuppressing migrations of intrinsic and extrinsic ions (e.g., Pb2+, I, FA+/MA+, and Li+) in organic–inorganic hybrid perovskites is critical for alleviating the hysteresis and degradation of perovskite solar cells (PSCs). However, various additives reported for that purpose usually interact with one or two types of those ions, not inhibiting multiple‐ion migrations simultaneously. Two oligosaccharides (β‐cyclodextrin (β‐CD) and maltotetraose (G4)), containing 14 hydroxyls (−OH) with different spatial distributions, for the suppression of multiple‐ion migrations in PSCs is herein employed. Compared to linear arrangement of −OH in G4, annular distribution of −OH around wide and narrow rims of β‐CD can form supramolecular multi‐site interactions in a focal manner with various ions, more effectively capturing and immobilizing these migrated ions. With this multiple‐ion management strategy, β‐CD‐based PSCs exhibit an impressive efficiency of 24.22% with negligible hysteresis and excellent device stability. This work highlights the significances of multi‐site interactions and molecular configuration of the additive for inhibiting multi‐ion migrations in PSCs.

Funder

National Natural Science Foundation of China

Liaoning Revitalization Talents Program

Natural Science Foundation of Shandong Province

Dalian Institute of Chemical Physics

Publisher

Wiley

Subject

Biomaterials,Biotechnology,General Materials Science,General Chemistry

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