Development of an Adrenocortical Cancer Humanized Mouse Model to Characterize Anti-PD1 Effects on Tumor Microenvironment

被引:40
|
作者
Lang, Julie [1 ]
Capasso, Anna [2 ]
Jordan, Kimberly R. [1 ]
French, Jena D. [3 ]
Kar, Adwitiya [3 ]
Bagby, Stacey M. [2 ]
Barbee, Jacob [1 ]
Yacob, Betelehem W. [2 ]
Head, Lia S. [2 ]
Tompkins, Kenneth D. [3 ]
Freed, Brian M. [1 ]
Somerset, Hilary [4 ]
Clark, Toshimasa J. [5 ]
Pitts, Todd M. [2 ]
Messersmith, Wells A. [2 ]
Eckhardt, S. Gail [7 ]
Wierman, Margaret E. [3 ,6 ]
Leong, Stephen [2 ]
Kiseljak-Vassiliades, Katja [3 ,6 ]
机构
[1] Univ Colorado, Dept Immunol & Microbiol, Sch Med, Anschutz Med Campus, Aurora, CO 80045 USA
[2] Univ Colorado, Div Med Oncol, Dept Med, Sch Med, Colorado Anschutz Med Campus, Aurora, CO 80045 USA
[3] Univ Colorado, Div Endocrinol Metab & Diabet, Dept Med, Sch Med, Colorado Anschutz Med Campus, Aurora, CO 80045 USA
[4] Univ Colorado, Dept Pathol, Sch Med, Colorado Anschutz Med Campus, Aurora, CO 80045 USA
[5] Univ Colorado, Dept Radiol, Sch Med, Colorado Anschutz Med Cam, Aurora, CO 80045 USA
[6] Res Serv Vet Affairs Med Ctr, Denver, CO 80220 USA
[7] Univ Texas Austin, Dell Med Sch, Austin, TX 78701 USA
来源
JOURNAL OF CLINICAL ENDOCRINOLOGY & METABOLISM | 2020年 / 105卷 / 01期
关键词
Adrenocortical carcinoma; anti-PD-1; humanized mouse PDX model; immunotherapy; MULTIPLEXED IMMUNOHISTOCHEMISTRY; XENOGRAFT MODELS; T-CELLS; CARCINOMA; MICE; NIVOLUMAB; RECONSTITUTION; IMMUNOTHERAPY; IPILIMUMAB; EXPRESSION;
D O I
10.1210/clinem/dgz014
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Context: Although the development of immune checkpoint inhibitors has transformed treatment strategies of several human malignancies, research models to study immunotherapy in adrenocortical carcinoma (ACC) are lacking. Objective: To explore the effect of anti-PD1 immunotherapy on the alteration of the immune milieu in ACC in a newly generated preclinical model and correlate with the response of the matched patient. Design, Setting, and Intervention: To characterize the CU-ACC2-M2B patient-derived xenograft in a humanized mouse model, evaluate the effect of a PD-1 inhibitor therapy, and compare it with the CU-ACC2 patient with metastatic disease. Results: Characterization of the CU-ACC2-humanized cord blood-BALB/c-Rag2(null)Il2r gamma(null)Sirpa(NOD) model confirmed ACC origin and match with the original human tumor. Treatment of the mice with pembrolizumab demonstrated significant tumor growth inhibition (60%) compared with controls, which correlated with increased tumor infiltrating lymphocyte activity, with an increase of human CD8(+) T cells (P < 0.05), HLA-DR+ T cells (P < 0.05) as well as Granzyme B+ CD8(+) T cells (<0.001). In parallel, treatment of the CU-ACC2 patient, who had progressive disease, demonstrated a partial response with 79% to 100% reduction in the size of target lesions, and no new sites of metastasis. Pretreatment analysis of the patient's metastatic liver lesion demonstrated abundant intratumoral CD8(+) T cells by immunohistochemistry. Conclusions: Our study reports the first humanized ACC patient-derived xenograft mouse model, which may be useful to define mechanisms and biomarkers of response and resistance to immune-based therapies, to ultimately provide more personalized care for patients with ACC.
引用
收藏
页码:26 / 42
页数:17
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