Multiple myeloma (MM) is an age-dependent hematological malignancy. Evaluation of immune interactions that drive MM relies on in vitro experiments that do not reflect the complex cellular stroma involved in MM pathogenesis. Here we used Vk*MYC transgenic mice, which spontaneously develop MM, and demonstrated that the immune system plays a critical role in the control of MM progression and the response to treatment. We monitored Vk*MYC mice that had been crossed with
Camille Guillerey, Lucas Ferrari de Andrade, Slavica Vuckovic, Kim Miles, Shin Foong Ngiow, Michelle C.R. Yong, Michele W.L. Teng, Marco Colonna, David S. Ritchie, Martha Chesi, P. Leif Bergsagel, Geoffrey R. Hill, Mark J. Smyth, Ludovic Martinet
Title and authors | Publication | Year |
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Combination cancer immunotherapy and new immunomodulatory targets
KM Mahoney, PD Rennert, GJ Freeman |
Nature Reviews Drug Discovery | 2015 |
Primary myeloma interaction and growth in coculture with healthy donor hematopoietic bone marrow
R Bam, S Khan, W Ling, SS Randal, X Li, B Barlogie, R Edmondson, S Yaccoby |
BMC Cancer | 2015 |
Activation of NK cells and disruption of PD-L1/PD-1 axis: two different ways for lenalidomide to block myeloma progression
M Giuliani, B Janji, G Berchem |
Oncotarget | 2015 |
The IMiDs targets IKZF-1/3 and IRF4 as novel negative regulators of NK cell-activating ligands expression in multiple myeloma
C Fionda, MP Abruzzese, A Zingoni, F Cecere, E Vulpis, G Peruzzi, A Soriani, R Molfetta, R Paolini, MR Ricciardi, MT Petrucci, A Santoni, M Cippitelli |
Oncotarget | 2015 |