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Enhancement of Local Piezoresponse in Polymer Ferroelectrics via Nanoscale Control of Microstructure

Author: Alexei Gruverman (1390405)
Byeongdu Lee (1273785)
Charudatta Phatak (1309107)
David J. Gosztola (1343949)
Jiangyu Li (1390402)
Joonseok Lee (1390399)
Pankaj Sharma (58141)
Seungbum Hong (1309119)
Stephen Ducharme (1301514)
Yoon-Young Choi (1390396)
Yunya Liu (1390393)
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Polymer ferroelectrics are flexible and lightweight electromechanical materials that are widely studied due to their potential application as sensors, actuators, and energy harvesters. However, one of the biggest challenges is their low piezoelectric coefficient. Here, we report a mechanical annealing effect based on local pressure induced by a nanoscale tip that enhances the local piezoresponse. This process can control the nanoscale material properties over a microscale area at room temperature. We attribute this improvement to the formation and growth of β-phase extended chain crystals via sliding diffusion and crystal alignment along the scan axis under high mechanical stress. We believe that this technique can be useful for local enhancement of piezoresponse in ferroelectric polymer thin films

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Image_1_Cas1 and Cas2 From the Type II-C CRISPR-Cas System of Riemerella anatipestifer Are Required for Spacer Acquisition.PDF

Author: Anchun Cheng (420072)
Chaoyue Liu (5372738)
Dekang Zhu (3926276)
Haibo Yi (1608802)
Li Huang (107408)
Ling Zhang (18071)
Mafeng Liu (3926267)
Mingshu Wang (3926270)
Qiao Yang (1506640)
Renyong Jia (420073)
Shaqiu Zhang (4392235)
Shun Chen (745877)
Xin Zhang (35492)
Xinxin Zhao (317779)
Yang He (307595)
Yanling Yu (2359852)
Ying Wu (4463161)
Yunya Liu (1390393)
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Clustered regularly interspaced short palindromic repeats (CRISPR) and CRISPR-associated (Cas) proteins provide acquired genetic immunity against the entry of mobile genetic elements (MGEs). The immune defense provided by various subtypes of the CRISPR-Cas system has been confirmed and is closely associated with the formation of immunological memory in CRISPR arrays, called CRISPR adaptation or spacer acquisition. However, whether type II-C CRISPR-Cas systems are also involved in spacer acquisition remains largely unknown. This study explores and provides some definitive evidence regarding spacer acquisition of the type II-C CRISPR-Cas system from Riemerella anatipestifer (RA) CH-2 (RA-CH-2). Firstly, introducing an exogenous plasmid into RA-CH-2 triggered spacer acquisition of RA CRISPR-Cas system, and the acquisition of new spacers led to plasmid instability in RA-CH-2. Furthermore, deletion of cas1 or cas2 of RA-CH-2 abrogated spacer acquisition and subsequently stabilized the exogenous plasmid, suggesting that both Cas1 and Cas2 are required for spacer acquisition of RA-CH-2 CRISPR-Cas system, consistent with the reported role of Cas1 and Cas2 in type I-E and II-A systems. Finally, assays for studying Cas1 nuclease activity and the interaction of Cas1 with Cas2 contributed to a better understanding of the adaptation mechanism of RA CRISPR-Cas system. This is the first experimental identification of the naïve adaptation of type II-C CRISPR-Cas system.</p

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