Establishment and characterization of NCC-MFS2-C1: a novel patient-derived cancer cell line of myxofibrosarcoma

“…We examined the antitumor effects of 210 drugs on NCC-MFS5-C1 cells. The cell viability of NCC-MFS5-C1 cells after drug treatment is summarized in Table S5 , along with the cell viabilities of NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ] cells, which we previously reported. The drugs were categorized into three groups according to their antitumor effect: cluster A, effective group; cluster B, intermediate effect group; cluster C, poor effect group ( Figure 4 a).…”

“…The IC 50 values of NCC-MFS5-C1 were calculated for the drugs that were hit in the screening study, and are summarized in Table S6 , along with those of NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ]. Notably, the proteasome inhibitor, bortezomib, and the histone deacetylase (HDAC) inhibitor, romidepsin, showed a more remarkable antitumor effect in all five MFS cell lines than doxorubicin, which is used as a standard drug for the treatment of sarcomas ( Figure 5 , Table 3 ).…”

“…Invasive potential was assessed using a real-time cell analyzer (xCELLigence, Agilent, Santa Clara, CA, USA) along with NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ], as previously reported [ 32 ]. We seeded cells (4 × 10 4 ) suspended in a serum-free DMEM/F12 medium in the upper chamber coated with BD Matrigel matrix (BD Biosciences, Franklin Lakes, NJ, USA) ( n = 2).…”

“…Cell viability was calculated by comparing with the DMSO control. The acquired data were analyzed using the results of NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ], which we previously reported. Quantile normalization was performed using R (version 4.0.3, limma package version 3.46.0, Bioconductor), and unsupervised hierarchical clustering was performed using the gplots package (version 3.1.0, CRAN, , accessed on 28 October 2021).…”

“…Thus, we established an MFS cell line and named it NCC-MFS5-C1 using surgical specimens of MFS. In addition to a detailed characterization of the cell line, we attempted to identify novel candidate drugs by integrating the results of drug screening studies for the following MFS cell lines, as reported in our previous studies: NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ].…”

Establishment and Characterization of NCC-MFS5-C1: A Novel Patient-Derived Cell Line of Myxofibrosarcoma

“…We examined the antitumor effects of 210 drugs on NCC-MFS5-C1 cells. The cell viability of NCC-MFS5-C1 cells after drug treatment is summarized in Table S5 , along with the cell viabilities of NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ] cells, which we previously reported. The drugs were categorized into three groups according to their antitumor effect: cluster A, effective group; cluster B, intermediate effect group; cluster C, poor effect group ( Figure 4 a).…”

“…The IC 50 values of NCC-MFS5-C1 were calculated for the drugs that were hit in the screening study, and are summarized in Table S6 , along with those of NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ]. Notably, the proteasome inhibitor, bortezomib, and the histone deacetylase (HDAC) inhibitor, romidepsin, showed a more remarkable antitumor effect in all five MFS cell lines than doxorubicin, which is used as a standard drug for the treatment of sarcomas ( Figure 5 , Table 3 ).…”

“…Invasive potential was assessed using a real-time cell analyzer (xCELLigence, Agilent, Santa Clara, CA, USA) along with NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ], as previously reported [ 32 ]. We seeded cells (4 × 10 4 ) suspended in a serum-free DMEM/F12 medium in the upper chamber coated with BD Matrigel matrix (BD Biosciences, Franklin Lakes, NJ, USA) ( n = 2).…”

“…Cell viability was calculated by comparing with the DMSO control. The acquired data were analyzed using the results of NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ], which we previously reported. Quantile normalization was performed using R (version 4.0.3, limma package version 3.46.0, Bioconductor), and unsupervised hierarchical clustering was performed using the gplots package (version 3.1.0, CRAN, , accessed on 28 October 2021).…”

“…Thus, we established an MFS cell line and named it NCC-MFS5-C1 using surgical specimens of MFS. In addition to a detailed characterization of the cell line, we attempted to identify novel candidate drugs by integrating the results of drug screening studies for the following MFS cell lines, as reported in our previous studies: NCC-MFS1-C1 [ 28 ], NCC-MFS2-C1 [ 29 ], NCC-MFS3-C1 [ 30 ], and NCC-MFS4-C1 [ 31 ].…”

Establishment and Characterization of NCC-MFS5-C1: A Novel Patient-Derived Cell Line of Myxofibrosarcoma

Establishment and characterization of NCC-MFS3-C1: a novel patient-derived cell line of myxofibrosarcoma

Establishment and characterization of NCC-MFS4-C1: a novel patient-derived cell line of myxofibrosarcoma