Literature DB >> 30129680

Dual use of hematopoietic and mesenchymal stem cells enhances engraftment and immune cell trafficking in an allogeneic humanized mouse model of head and neck cancer.

John J Morton1, Stephen B Keysar1, Loni Perrenoud1, Tugs-Saikhan Chimed1, Julie Reisinger1, Brian Jackson1, Phuong N Le1, Cera Nieto1, Karina Gomez1, Bettina Miller1, Dexiang Gao2, Hilary Somerset3, Xiao-Jing Wang3,4,5, Antonio Jimeno1,4.   

Abstract

In this report, we describe in detail the evolving procedures to optimize humanized mouse cohort generation, including optimal conditioning, choice of lineage for engraftment, threshold for successful engraftment, HNSCC tumor implantation, and immune and stroma cell analyses. We developed a dual infusion protocol of human hematopoietic stem and progenitor cells (HSPCs) and mesenchymal stem cells (MSCs), leading to incremental human bone marrow engraftment, and exponential increase in mature peripheral human immune cells, and intratumor homing that includes a more complete lineage reconstitution. Additionally, we have identified practical rules to predict successful HSPC/MSC expansion, and a peripheral human cell threshold associated with bone marrow engraftment, both of which will optimize cohort generation and management. The tremendous advances in immune therapy in cancer have made the need for appropriate and standardized models more acute than ever, and therefore, we anticipate that this manuscript will have an immediate impact in cancer-related research. The need for more representative tools to investigate the human tumor microenvironment (TME) has led to the development of humanized mouse models. However, the difficulty of immune system engraftment and minimal human immune cell infiltration into implanted xenografts are major challenges. We have developed an improved method for generating mismatched humanized mice (mHM), using a dual infusion of human HSPCs and MSCs, isolated from cord blood and expanded in vitro. Engraftment with both HSPCs and MSCs produces mice with almost twice the percentage of human immune cells in their bone marrow, compared to mice engrafted with HSPCs alone, and yields 9- to 38-fold higher levels of mature peripheral human immune cells. We identified a peripheral mHM blood human B cell threshold that predicts an optimal degree of mouse bone marrow humanization. When head and neck squamous cell carcinoma (HNSCC) tumors are implanted on the flanks of HSPC-MSC engrafted mice, human T cells, B cells, and macrophages infiltrate the stroma of these tumors at 2- to 8-fold higher ratios. In dually HSPC-MSC engrafted mice we also more frequently observed additional types of immune cells, including regulatory T cells, cytotoxic T cells, and MDSCs. Higher humanization was associated with in vivo response to immune-directed therapy. The complex immune environment arising in tumors from dually HSPC-MSC engrafted mice better resembles that of the originating patient's tumor, suggesting an enhanced capability to accurately recapitulate a human TME.
© 2018 Wiley Periodicals, Inc.

Entities:  

Keywords:  cancer microenvironment; head and neck cancer; hematopoietic stem cell; humanized mouse model; patient-derived xenograft

Mesh:

Substances:

Year:  2018        PMID: 30129680      PMCID: PMC6452868          DOI: 10.1002/mc.22887

Source DB:  PubMed          Journal:  Mol Carcinog        ISSN: 0899-1987            Impact factor:   4.784


  37 in total

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Journal:  Clin Immunol       Date:  2015-02-25       Impact factor: 3.969

Review 2.  Humanized mice in translational biomedical research.

Authors:  Leonard D Shultz; Fumihiko Ishikawa; Dale L Greiner
Journal:  Nat Rev Immunol       Date:  2007-02       Impact factor: 53.106

Review 3.  Concise review: humanized models of tumor immunology in the 21st century: convergence of cancer research and tissue engineering.

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Journal:  Stem Cells       Date:  2015-06       Impact factor: 6.277

4.  Human lymphoid and myeloid cell development in NOD/LtSz-scid IL2R gamma null mice engrafted with mobilized human hemopoietic stem cells.

Authors:  Leonard D Shultz; Bonnie L Lyons; Lisa M Burzenski; Bruce Gott; Xiaohua Chen; Stanley Chaleff; Malak Kotb; Stephen D Gillies; Marie King; Julie Mangada; Dale L Greiner; Rupert Handgretinger
Journal:  J Immunol       Date:  2005-05-15       Impact factor: 5.422

Review 5.  Current advances in humanized mouse models.

Authors:  Ryoji Ito; Takeshi Takahashi; Ikumi Katano; Mamoru Ito
Journal:  Cell Mol Immunol       Date:  2012-02-13       Impact factor: 11.530

Review 6.  The role of tumour-stromal interactions in modifying drug response: challenges and opportunities.

Authors:  Douglas W McMillin; Joseph M Negri; Constantine S Mitsiades
Journal:  Nat Rev Drug Discov       Date:  2013-03       Impact factor: 84.694

7.  XactMice: humanizing mouse bone marrow enables microenvironment reconstitution in a patient-derived xenograft model of head and neck cancer.

Authors:  J J Morton; G Bird; S B Keysar; D P Astling; T R Lyons; R T Anderson; M J Glogowska; P Estes; J R Eagles; P N Le; G Gan; B McGettigan; P Fernandez; N Padilla-Just; M Varella-Garcia; J I Song; D W Bowles; P Schedin; A-C Tan; D R Roop; X-J Wang; Y Refaeli; A Jimeno
Journal:  Oncogene       Date:  2015-04-20       Impact factor: 9.867

8.  A Humanized Mouse Model Generated Using Surplus Neonatal Tissue.

Authors:  Matthew E Brown; Ying Zhou; Brian E McIntosh; Ian G Norman; Hannah E Lou; Mitch Biermann; Jeremy A Sullivan; Timothy J Kamp; James A Thomson; Petros V Anagnostopoulos; William J Burlingham
Journal:  Stem Cell Reports       Date:  2018-03-22       Impact factor: 7.765

9.  Patient-derived xenografts undergo mouse-specific tumor evolution.

Authors:  Uri Ben-David; Gavin Ha; Yuen-Yi Tseng; Noah F Greenwald; Coyin Oh; Juliann Shih; James M McFarland; Bang Wong; Jesse S Boehm; Rameen Beroukhim; Todd R Golub
Journal:  Nat Genet       Date:  2017-10-09       Impact factor: 38.330

Review 10.  Humanized Mice as Unique Tools for Human-Specific Studies.

Authors:  Kylie Su Mei Yong; Zhisheng Her; Qingfeng Chen
Journal:  Arch Immunol Ther Exp (Warsz)       Date:  2018-02-07       Impact factor: 4.291

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  5 in total

1.  Cancer Cell CD44 Mediates Macrophage/Monocyte-Driven Regulation of Head and Neck Cancer Stem Cells.

Authors:  Karina E Gomez; FangLong Wu; Stephen B Keysar; J Jason Morton; Bettina Miller; Tugs-Saikhan Chimed; Phuong N Le; Cera Nieto; Farshad N Chowdhury; Anit Tyagi; Traci R Lyons; Christian D Young; Hongmei Zhou; Hilary L Somerset; Xiao-Jing Wang; Antonio Jimeno
Journal:  Cancer Res       Date:  2020-08-14       Impact factor: 12.701

Review 2.  Myeloid-Derived Suppressor Cells (MDSC) in the Umbilical Cord Blood: Biological Significance and Possible Therapeutic Applications.

Authors:  Nikoleta Bizymi; Anthie Georgopoulou; Natalia Mastrogamvraki; Angelos Matheakakis; Ioanna Gontika; Irene Fragiadaki; Irene Mavroudi; Helen A Papadaki
Journal:  J Clin Med       Date:  2022-01-29       Impact factor: 4.241

Review 3.  Mouse Models for Immune Checkpoint Blockade Therapeutic Research in Oral Cancer.

Authors:  Wei-Chiao Chiu; Da-Liang Ou; Ching-Ting Tan
Journal:  Int J Mol Sci       Date:  2022-08-16       Impact factor: 6.208

4.  Studying Immunotherapy Resistance in a Melanoma Autologous Humanized Mouse Xenograft.

Authors:  J Jason Morton; Nathaniel Alzofon; Stephen B Keysar; Tugs-Saikhan Chimed; Julie Reisinger; Loni Perrenoud; Phuong N Le; Cera Nieto; Karina Gomez; Bettina Miller; Randi Yeager; Dexiang Gao; Aik-Choon Tan; Hilary Somerset; Theresa Medina; Xiao-Jing Wang; Jing H Wang; William Robinson; Dennis R Roop; Rene Gonzalez; Antonio Jimeno
Journal:  Mol Cancer Res       Date:  2020-10-21       Impact factor: 6.333

Review 5.  Mouse Tumor-Bearing Models as Preclinical Study Platforms for Oral Squamous Cell Carcinoma.

Authors:  Qiang Li; Heng Dong; Guangwen Yang; Yuxian Song; Yongbin Mou; Yanhong Ni
Journal:  Front Oncol       Date:  2020-02-25       Impact factor: 6.244

  5 in total

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