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kpc cell line (CancerTools Org)

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CancerTools Org kpc cell line
Kpc Cell Line, supplied by CancerTools Org, used in various techniques. Bioz Stars score: 99/100, based on 306 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/kpc cell line/product/CancerTools Org
Average 99 stars, based on 306 article reviews

kpc cell line - by Bioz Stars, 2026-06

99/100 stars

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kpc cells (Absolute Biotech Inc)

Absolute Biotech Inc kpc cells

( a, b ) Peripheral blood immune profiling in the <t>KPC</t> flank model. <t>KPC</t> <t>cells</t> (1.0 x 10 6 ) cells were inoculated into the right flanks of 6-8-week-old C57BL/6J mice. Once tumors reach the target volume of 80-120 mm³ mice were randomized to treatment group (n=8/group) and treated with PBS or lyophilized iSTORM (iSTORM-L) at 5×10 7 CFU or 1×10 8 CFU/mouse, administered intraperitoneally, one bolus every 3 days, 4 doses total). Immune profiling in peripheral blood collected 15/16 days post the last treatment (23/24 days after the first dose) demonstrates that iSTROM fully retains immune-stimulatory activities and elicits a graded, dose-dependent activation of circulating T-cell compartments. Increasing iSTORM-L doses expanded activated CD4 + T cells (CD44 + CD69 + and ICOS + ) while concomitantly reducing exhaustion-associated PD-1 + and PD-1 + LAG3 + CD4 + subsets ( a ). CD8 + T cells displayed a parallel activation program, characterized by robust expansion of ICOS⁺ effector-like CD8 + T cells and uniformly low frequencies of PD-1 + or PD-1 + TIM3 + exhausted populations across all doses ( b ). c ) iSTORM-L induced dose-dependent tumor growth suppression in the KPC mice above. Tumor volumes (caliper measurements) were measured twice per week. Bar and whisker represent means and standard deviation, respectively.

Kpc Cells, supplied by Absolute Biotech Inc, used in various techniques. Bioz Stars score: 86/100, based on 1 PubMed citations. ZERO BIAS - scores, article reviews, protocol conditions and more
https://www.bioz.com/result/kpc cells/product/Absolute Biotech Inc
Average 86 stars, based on 1 article reviews

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( a, b ) Peripheral blood immune profiling in the KPC flank model. KPC cells (1.0 x 10 6 ) cells were inoculated into the right flanks of 6-8-week-old C57BL/6J mice. Once tumors reach the target volume of 80-120 mm³ mice were randomized to treatment group (n=8/group) and treated with PBS or lyophilized iSTORM (iSTORM-L) at 5×10 7 CFU or 1×10 8 CFU/mouse, administered intraperitoneally, one bolus every 3 days, 4 doses total). Immune profiling in peripheral blood collected 15/16 days post the last treatment (23/24 days after the first dose) demonstrates that iSTROM fully retains immune-stimulatory activities and elicits a graded, dose-dependent activation of circulating T-cell compartments. Increasing iSTORM-L doses expanded activated CD4 + T cells (CD44 + CD69 + and ICOS + ) while concomitantly reducing exhaustion-associated PD-1 + and PD-1 + LAG3 + CD4 + subsets ( a ). CD8 + T cells displayed a parallel activation program, characterized by robust expansion of ICOS⁺ effector-like CD8 + T cells and uniformly low frequencies of PD-1 + or PD-1 + TIM3 + exhausted populations across all doses ( b ). c ) iSTORM-L induced dose-dependent tumor growth suppression in the KPC mice above. Tumor volumes (caliper measurements) were measured twice per week. Bar and whisker represent means and standard deviation, respectively.

Journal: bioRxiv

Article Title: CMTM6-Silencing Microbial Immunotherapy Reprograms PDAC Tumors and Restores T-cell Function

doi: 10.64898/2026.01.26.701790

Figure Lengend Snippet: ( a, b ) Peripheral blood immune profiling in the KPC flank model. KPC cells (1.0 x 10 6 ) cells were inoculated into the right flanks of 6-8-week-old C57BL/6J mice. Once tumors reach the target volume of 80-120 mm³ mice were randomized to treatment group (n=8/group) and treated with PBS or lyophilized iSTORM (iSTORM-L) at 5×10 7 CFU or 1×10 8 CFU/mouse, administered intraperitoneally, one bolus every 3 days, 4 doses total). Immune profiling in peripheral blood collected 15/16 days post the last treatment (23/24 days after the first dose) demonstrates that iSTROM fully retains immune-stimulatory activities and elicits a graded, dose-dependent activation of circulating T-cell compartments. Increasing iSTORM-L doses expanded activated CD4 + T cells (CD44 + CD69 + and ICOS + ) while concomitantly reducing exhaustion-associated PD-1 + and PD-1 + LAG3 + CD4 + subsets ( a ). CD8 + T cells displayed a parallel activation program, characterized by robust expansion of ICOS⁺ effector-like CD8 + T cells and uniformly low frequencies of PD-1 + or PD-1 + TIM3 + exhausted populations across all doses ( b ). c ) iSTORM-L induced dose-dependent tumor growth suppression in the KPC mice above. Tumor volumes (caliper measurements) were measured twice per week. Bar and whisker represent means and standard deviation, respectively.

Article Snippet: KPC cells (Kerafast, catalog# EUP012-FP, MA, United States) were maintained in DMEM-High Glucose (Gibco TM , catalog# 11965092, NY, United States) supplemented with 10% FBS (Sigma-Aldrich, catalog# F4135, MO, United States).

Techniques: Activation Assay, Whisker Assay, Standard Deviation