Human mesenchymal stem cells increase LLC metastasis and stimulate or decelerate tumor development depending on injection method and cell amount

Yurii V Stepanov; Iuliia Golovynska; Galyna Ostrovska; Larysa Pylyp; Taisa Dovbynchuk; Liudmyla I Stepanova; Oleksandr Gorbach; Volodymyr Shablii; Hao Xu; Liudmyla V Garmanchuk; Tymish Y Ohulchanskyy; Junle Qu; Galina I Solyanik

doi:10.1002/cyto.a.24814

Human mesenchymal stem cells increase LLC metastasis and stimulate or decelerate tumor development depending on injection method and cell amount

Cytometry A. 2024 Apr;105(4):252-265. doi: 10.1002/cyto.a.24814. Epub 2024 Jan 16.

Authors

Affiliations

¹ Shenzhen Key Laboratory of Photonics and Biophotonics, College of Physics and Optoelectronic Engineering, Shenzhen University, Shenzhen, People's Republic of China.
² Laboratory of Molecular and Cellular Mechanisms of Metastasis, R.E. Kavetsky Institute of Experimental Pathology, Oncology and Radiobiology, NAS of Ukraine, Kyiv, Ukraine.
³ Institute of Biology and Medicine, Taras Shevchenko National University of Kyiv, Kyiv, Ukraine.
⁴ Clinic of Reproductive Medicine "Nadiya", Kyiv, Ukraine.
⁵ Laboratory of Experimental Oncology, National Cancer Institute of Ukraine, Kyiv, Ukraine.
⁶ Institute of Molecular Biology and Genetics, NAS of Ukraine, Kyiv, Ukraine.
⁷ Institute of Cell Therapy, Kyiv, Ukraine.

PMID: 38038631
DOI: 10.1002/cyto.a.24814

Abstract

Mesenchymal stem cells (MSCs) being injected into the body can stimulate or decelerate carcinogenesis. Here, the direction of influence of human placenta-derived MSCs (P-MSCs) on the Lewis lung carcinoma (LLC) tumor development and metastatic potential is investigated in C57BL/6 mice depending on the injection method. After intramuscular co-inoculation of LLC and P-MSCs (LLC + P-MSCs), the growth of primary tumor and angiogenesis are slowed down compared to the control LLC on the 15th day. This is explained by the fact of a decrease in the secretion of proangiogenic factors during in vitro co-cultivation of an equal amount of LLC and P-MSCs. When P-MSCs are intravenously (i.v.) injected in the mice with developing LLC (LLC + P-MSCs(i.v.)), the tumor growth and angiogenesis are stimulated on the 15th day. A highly activated secretion of proangiogenic factors by P-MSCs in a similar in vitro model can explain this. In both the models compared to the control on the 23rd day, there is no significant difference in the tumor growth, while angiogenesis remains correspondingly decelerated or stimulated. However, in both the models, the total volume and number of lung metastases constantly increase compared to the control: it is mainly due to small-size metastases for LLC + P-MSCs(i.v.) and larger ones for LLC + P-MSCs. The increase in the rate of LLC cell dissemination after the injection of P-MSCs is explained by the disordered polyploidy and chromosomal instability, leading to an increase in migration and invasion of cancer cells. After LLC + P-MSCs co-inoculation, the tumor cell karyotype has the most complex and heterogeneous chromosomal structure. These findings indicate a bidirectional effect of P-MSCs on the growth of LLC in the early periods after injection, depending on the injection method, and, correspondingly, the number of contacting cells. However, regardless of the injection method, P-MSCs are shown to increase LLC aggressiveness related to cancer-associated angiogenesis and metastasis activation in the long term.

Keywords: Lewis lung carcinoma karyotype; angiogenesis; cancer; human mesenchymal stem cells; tumor growth and metastasis.

MeSH terms

Animals
Carcinoma, Lewis Lung* / pathology
Humans
Lung Neoplasms* / pathology
Mesenchymal Stem Cells*
Mice
Mice, Inbred C57BL

Abstract

MeSH terms

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