surfactant composition
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Langmuir ◽  
2021 ◽  
Author(s):  
Trang Vu ◽  
Geoffrey Reynolds ◽  
Howard D. Hutton ◽  
Gerald B. Kasting ◽  
Peter Koenig

2020 ◽  
Vol Volume 15 ◽  
pp. 8767-8781
Author(s):  
Morteza Yaghoobian ◽  
Azadeh Haeri ◽  
Noushin Bolourchian ◽  
Soraya Shahhosseni ◽  
Simin Dadashzadeh

Micromachines ◽  
2020 ◽  
Vol 11 (7) ◽  
pp. 701 ◽  
Author(s):  
Shougo Fujiwara ◽  
Kan Shoji ◽  
Chiho Watanabe ◽  
Ryuji Kawano ◽  
Miho Yanagisawa

Assembled water-in-oil droplets bounded by lipid bilayers are used in synthetic biology as minimal models of cell tissue. Microfluidic devices successfully generate monodispersed droplets and assemble them via droplet interface bilayesr (DIB) formation. However, a honeycomb pattern of DIB-bounded droplets, similar to epithelial tissues, remains unrealized because the rapid DIB formation between the droplets hinders their ability to form the honeycomb pattern. In this paper, we demonstrate the microfluidic formation of a honeycomb pattern of DIB-bounded droplets using two surfactants with different adsorption rates on the droplet surface. A non-DIB forming surfactant (sorbitan monooleate, Span 80) was mixed with a lipid (1,2-dioleoyl-sn-glycero-3-phosphocholine, PC), whose adsorption rate on the droplet surface and saturated interfacial tension were lower than those of Span 80. By changing the surfactant composition, we established the conditions under which the droplets initially form a honeycomb pattern and subsequently adhere to each other via DIB formation to minimize the interfacial energy. In addition, the reconstituted membrane protein nanopores at the DIBs were able to transport molecules. This new method, using the difference in the adsorption rates of two surfactants, allows the formation of a honeycomb pattern of DIB-bounded droplets in a single step, and thus facilitates research using DIB-bounded droplet assemblies.


2020 ◽  
Vol 215 ◽  
pp. 115370
Author(s):  
Mengmeng Yang ◽  
Yiyu Lu ◽  
Zhaolong Ge ◽  
Zhe Zhou ◽  
Chengjuan Chai ◽  
...  

Author(s):  
Trang Vu ◽  
Peter Koenig ◽  
Brooke M. Cochran ◽  
K.P. Ananthapadmanabhan ◽  
Mike Weaver ◽  
...  

Author(s):  
Anna-Carin Olin ◽  
Spela Kokelj ◽  
Ekaterina Mirgorodskaya ◽  
Christer Jansson ◽  
Mathias Holm ◽  
...  

2019 ◽  
Vol 5 (9) ◽  
pp. eaaw6671 ◽  
Author(s):  
Matthias Huelsmann ◽  
Nikolai Hecker ◽  
Mark S. Springer ◽  
John Gatesy ◽  
Virag Sharma ◽  
...  

The transition from land to water in whales and dolphins (cetaceans) was accompanied by remarkable adaptations. To reveal genomic changes that occurred during this transition, we screened for protein-coding genes that were inactivated in the ancestral cetacean lineage. We found 85 gene losses. Some of these were likely beneficial for cetaceans, for example, by reducing the risk of thrombus formation during diving (F12 and KLKB1), erroneous DNA damage repair (POLM), and oxidative stress–induced lung inflammation (MAP3K19). Additional gene losses may reflect other diving-related adaptations, such as enhanced vasoconstriction during the diving response (mediated by SLC6A18) and altered pulmonary surfactant composition (SEC14L3), while loss of SLC4A9 relates to a reduced need for saliva. Last, loss of melatonin synthesis and receptor genes (AANAT, ASMT, and MTNR1A/B) may have been a precondition for adopting unihemispheric sleep. Our findings suggest that some genes lost in ancestral cetaceans were likely involved in adapting to a fully aquatic lifestyle.


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