ABSTRACT
Drug development is a time-consuming and expensive process, given the low success rate of clinical trials. Now, anticancer drug developments have shifted to three-dimensional (3D) models which are more likely to mimic tumor behavior compared to traditional two-dimensional (2D) cultures. A comparative study among different aspects was conducted between 2D and 3D cultures using colorectal cancer (CRC) cell lines, in addition, Formalin-Fixed Paraffin-Embedded (FFPE) block samples of patients with CRC were used for evaluation. Compared to the 2D culture, cells grown in 3D displayed significant (p < 0.01) differences in the pattern of cell proliferation over time, cell death phase profile, expression of tumorgenicity-related genes, and responsiveness to 5-fluorouracil, cisplatin, and doxorubicin. Epigenetically, 3D cultures and FFPE shared the same methylation pattern and microRNA expression, while 2D cells showed elevation in methylation rate and altered microRNA expression. Lastly, transcriptomic study depending on RNA sequencing and thorough bioinformatic analyses showed significant (p-adj < 0.05) dissimilarity in gene expression profile between 2D and 3D cultures involving thousands of genes (up/down-regulated) of multiple pathways for each cell line. Taken together, the study provides insights into variations in cellular morphologies between cells cultured in 2D and 3D models.
Subject(s)
Colorectal Neoplasms , MicroRNAs , Humans , Transcriptome , Cell Culture Techniques/methods , Cisplatin , Cell Proliferation/genetics , MicroRNAs/genetics , Colorectal Neoplasms/genetics , Colorectal Neoplasms/pathology , Cell Line, TumorABSTRACT
We systematically vary the nanoparticle (NP) dispersion state in composites formed by mixing polyisoprene homopolymers with polyisoprene grafted silica particles, and demonstrate how creep measurements allow us to overcome the limitations of small amplitude oscillatory shear (SAOS) experiments. This allows us to access nearly 13 orders in time in the mechanical response of the resulting composites. We find that a specific NP morphology, a percolating particle network achieved at intermediate graft densities, significantly reinforces the system and has a lower NP percolation loading threshold relative to other morphologies. These important effects of morphology only become apparent when we combine creep measurements with SAOS re-emphasizing the role of synergistically combining methods to access the mechanical properties of polymer nanocomposites over broad frequency ranges.
Subject(s)
Nanocomposites , Nanoparticles , Silicon Dioxide , PolymersABSTRACT
We rationalize the unusual gas transport behavior of polymer-grafted nanoparticle (GNP) membranes. While gas permeabilities depend specifically on the chemistry of the polymers considered, we focus here on permeabilities relative to the corresponding pure polymer which show interesting, "universal" behavior. For a given NP radius, Rc, and for large enough areal grafting densities, σ, to be in the dense brush regime we find that gas permeability enhancements display a maximum as a function of the graft chain molecular weight, Mn. Based on a recently proposed theory for the structure of a spherical brush in a melt of GNPs, we conjecture that this peak permeability occurs when the densely grafted polymer brush has the highest, packing-induced extension free energy per chain. The corresponding brush thickness is predicted to be h max = 3 R c , independent of chain chemistry and σ, i.e., at an apparently universal value of the NP volume fraction (or loading), ÏNP, ÏNP,max = [Rc/(Rc + hmax)]3 ≈ 0.049. Motivated by this conclusion, we measured CO-2 and CH4 permeability enhancements across a variety of Rc, Mn and σ, and find that they behave in a similar manner when considered as a function of ÏNP, with a peak in the near vicinity of the predicted ÏNP,max. Thus, the chain length dependent extension free energy appears to be the critical variable in determining the gas permeability for these hybrid materials. The emerging picture is that these curved polymer brushes, at high enough σ behave akin to a two-layer transport medium - the region in the near vicinity of the NP surface is comprised of extended polymer chains which speed-up gas transport relative to the unperturbed melt. The chain extension free energy increases with increasing chain length, up to a maximum, and apparently leads to an increasing gas permeability. For long enough grafts, there is an outer region of chain segments that is akin to an unperturbed melt with slow gas transport. The permeability maximum and decreasing permeability with increasing chain length then follow naturally.
ABSTRACT
Polymer membranes are critical to many sustainability applications that require the size-based separation of gas mixtures. Despite their ubiquity, there is a continuing need to selectively affect the transport of different mixture components while enhancing mechanical strength and hindering aging. Polymer-grafted nanoparticles (GNPs) have recently been explored in the context of gas separations. Membranes made from pure GNPs have higher gas permeability and lower selectivity relative to the neat polymer because they have increased mean free volume. Going beyond this ability to manipulate the mean free volume by grafting chains to a nanoparticle, the conceptual advance of the present work is our finding that GNPs are spatially heterogeneous transport media, with this free volume distribution being easily manipulated by the addition of free polymer. In particular, adding a small amount of appropriately chosen free polymer can increase the membrane gas selectivity by up to two orders of magnitude while only moderately reducing small gas permeability. Added short free chains, which are homogeneously distributed in the polymer layer of the GNP, reduce the permeability of all gases but yield no dramatic increases in selectivity. In contrast, free chains with length comparable to the grafts, which populate the interstitial pockets between GNPs, preferentially hinder the transport of the larger gas and thus result in large selectivity increases. This work thus establishes that we can favorably manipulate the selective gas transport properties of GNP membranes through the entropic effects associated with the addition of free chains.
