Review of Premetastasis Niche Research Progress

In recent years, the field of premetastasis niche has attracted more and more attention from international scholars and has become a hot research direc-tion. This article summarizes the current research on the role of the premetastasis niche, the components and formation mechanisms of the premetastasis niche, and the research on the significance of the premetastasis niche to the clinic. Effective cancer diagnosis and treatment strategies are important. A series of research advances in this field are of great significance for further elucidating the mechanism of tumor metastasis and designing more effective cancer diagnosis and treatment strategies.


Introduction
The tumor microenvironment is a complex and comprehensive system, which is composed of many stromal cells, including fibroblasts, immune and inflammatory cells, adipocytes, glial cells, smooth muscle cells, and some vascular cells. The most common immune cells in the tumor microenvironment are tumor-associated macrophages (TAM) [1].
The tumor creates a microenvironment suitable for metastasis in the distant organ, that is the premetastasis niche [2]. Metastatic microenvironment is a tumor produced by the complex interaction of tumor-derived factors, tumor-mobilized bone marrow-derived cells, and host primary stromal cells. This article summa-

Research on the Function of Premetastasis Niche
Metastasis refers to the migration of tumor cells to an area that is not directly adjacent to the primary tumor. Tumor cells can spread through blood and lymphatic vessels, or penetrate directly into the spaces and spread around organs.
Metastasis is a multi-stage process that requires tumor cells to shed from the primary foci, survive in circulation and grow in distant locations. Every stage of this process is affected by the tumor cells themselves and the tumor microenvironment. Some people believe that metastasis is a late-onset event in tumor development and is related to tumor volume [3]. More and more research evidences showed that the primary tumor can induce the formation of the second organ supportive microenvironment (pre-metastatic microenvironment), thereby promoting tumor metastasis [4] [5] [6]. The primary tumor will create a favorable microenvironment for the subsequent tumor metastasis in the distant organ or tissue, that is the pre-metastatic microenvironment. The formation of the premetastasis niche requires the interaction of tumor-derived factors, bone marrow-derived cells mobilized by the tumor, and local mesenchymal cells.
Proteases in the microenvironment provide a material basis for tumor metastasis. Tumor metastasis is accompanied by a variety of proteolytic activation, and this process is performed by a series of protein kinases, which is widely accepted. The matrix metalloproteinase (MMP) family is currently the most widely studied and considered to be the most closely related protease in tumors, because it is often up-regulated in tumors and can degrade ECM after secretion or localization on the cell surface, thus destroy the histological barrier of tumor cell invasion [3]. Hematopoietic stem cells overexpressing MMP9 induce malignant transformation of normal tissues and establish a pre-metastatic microenvironment, pre-metastatic niche plays an important role. The expression and secretion of MMP9 are regulated by VEGF and the chemokine ligand CXCL12/receptor CXCR4 axis, and the last two of them are also important factors that constitute the pre-metastatic microenvironment [7]. At the same time, CAF can secrete factor-1, SDF-1), etc. [7]. Recently, other proteases that make up the tumor microenvironment have gradually received more attention. For example, the cathepsin family, which functions similarly to MMPs, and some members are often up-regulated during tumorigenesis. Once localized on the cell surface, can also break down ECM and promote tumor metastasis [9].
Cathepsin is generally stable in the acidic environment of lysosomes and is capable of breaking down a range of substrates. In addition, there is evidence that cathepsin can also play a role in cells (such as cytosol, nucleus), cell surface and extracellular cells [10]. Both intracellular and extracellular cathepsin can cleave the major components of ECM and basement membrane, such as Laminin, Fibronectin and Collagentype IV, thereby promoting tumor cell infiltration and metastasis [11]. Although most cathepsin is constitutively expressed and functions in the lysosome, some cathepsin are overexpressed in tumor cells (such as cathepsin H, cathepsin L), and some are induced in non-tumor cells that constitute the tumor microenvironment. Some studies have investigated the potential application value of microenvironment before tumor metastasis and re-tumor prevention and treatment, the research mainly discussed in two aspects: 1) By blocking the generation of molecules that are beneficial to the formation of microenvironment before tumor metastasis; 2) Finding biomarkers that can predict tumor metastasis [12] (as shown in Figure 1). Figure 1. Role of the pre-metastatic niche in the promotion of tumor [12].

Research on the Formation Mechanism of Premetastasis Niche
This paper describes the molecular and cellular composition of the microenvironment before tumor metastasis and its regulatory mechanisms. In situ tumors can induce the formation of a microenvironment that is conducive to tumor cell metastasis in specific organs and tissues before metastasis. The formation of the microenvironment before tumor metastasis requires tumor secretion factors, mobilization of suppressive immune cells, and matrix components of the tissue site.
The interaction of three major factors, including inflammatory polarization. In addition, local hypoxia and extracellular matrix remodeling also promote the formation of a microenvironment before tumor metastasis. At the same time, the article comprehensively summarizes the key molecules and cellular components that promote the formation of the microenvironment before tumor metastasis and the underlying mechanisms, and first proposes six characteristics of the microenvironment before tumor metastasis: immunosuppression, inflammatory response, angiogenesis and permeability. Enhancement, lymphangiogenesis, pro-organism, and reprogramming provide new insights into the mechanism of the pre-metastatic microenvironment to promote tumor metastasis [12]. Each of the six features of the tumor process, including tumor metastasis, can be cleared by the immune system. CD8 + T cells, natural killer cells (NK), and atypical monocytes can prevent tumor metastasis without affecting the growth of the primary tumor [13]. Bone marrow-derived suppressor cells that accumulate in the premetastasis niche can also pass ARG1 and production of reactive oxygen species (ROS) inhibits anti-tumor T cells [14].
TNF receptor-2 can support bone marrow-derived suppressor cell-mediated immunosuppressive processes, promote tumor cell planting, growth and metastasis in the formation of a microenvironment before liver metastasis [15]. In lung, bone marrow, a large increase in immuno suppressive and metastasis-promoting T-regulatory cells has been demonstrated in a variety of cancers [16]. Metastatic cells in the tissue such as alveolar macrophages pretreated by breast cancer cells, can establish an immunosuppressive microenvironment by suppressing anti-tumor T cells [17]. Chronic inflammation is an important factor in tumor development and metastasis. There are many molecular components and signaling pathways involved in regulating immune cells, inflammation, tumor growth and metastasis.
For example, abnormal activation of TLR4 signaling in tumor cells can lead to inflammatory responses, tumor cell death resistance, and increase their proliferation and invasion capabilities. Similarly, abnormal activation of TLR4 and other innate immune cell sensing pathways leads to an inflammatory response that promotes tumor progression and metastasis [18]. TNF-α-induced S100A8-SAA3-TLR4 signaling pathway can also stimulate clara cells, thereby expressing SAA3 and maintaining the inflammatory state of the microenvironment before lung metastasis, to promote the occurrence of tumor lung met astasis [19].
CD11b + Gr-1 + cells in the microenvironment before lung metastasis can also  [19]. Upregulation of IL-6 by TLR5 and the hypoxic environment in the pre-metastatic microenvironment can drive tumor-promoted inflammatory responses. Therefore, before circulating tumor cells reach the site of metastasis, an inflammatory environment is established in the secondary site [20], which is conducive to the planting, survival, and proliferation of tumor cells in the premetastasis niche.
Enhanced angiogenesis and permeability, the microenvironment prior to metastasis may increase angiogenesis and vascular permeability, thereby promoting metastasis. TIE2 + monocytes and endothelial progenitor cells recruited in the pre-metastatic microenvironment to create a pro-stimulatory agent with high concentrations of VEGF and other pro-angiogenic factors.
The microenvironment of angiogenesis can initiate angiogenesis and promote the metastatic process in tumor progression [20]. In the pre-metastatic microenvironment, calcium-dependent phosphatase and activated T cell nuclear factor (NFAT) pathways can be specifically activated by lung endothelium before tumor cells arrive, due to NFAT-targeted angiogenin-2 (ANG-2), Leading to an increase in lung metastasis [21]. In the early formation of the premetastasis niche, miR105 secreted by metastatic breast cancer cells can damage the vascular endothelial barrier through tight junction of targeted cell tight junction proteins, thereby enhancing vascular permeability of distant organs and promoting metastasis [22]. In addition, the epidermal growth factor receptor ligand epidermal regulator, cyclooxygenase-2, MMP-1 and MMP-2 expressed by breast cancer cells recombine a multifunctional vascular remodeling program to increase vascular permeability and promote Pulmonary metastasis process [23].
Lymphangiogenesis in the premetastasis niche is an active step in tumor metastasis, and lymphatic vessels may serve as a starting site for lymphatic dissemination of tumors. Clinical data show that tumor-derived VEGF-A and VEGF-D generate lymphatic vessels before lymph node-induced metastasis, and are associated with lymph node metastasis [24]. The mechanism of lymphatic metastasis,  Figure 2).

Research on the Clinical Significance of Premetastasis Niche
Studies have shown that in a mouse model of breast cancer, the spread of tumor cells has nothing to do with tumor size, and it has occurred before tumor invasion. In addition, even non-malignant positive mammary epidermal cells can survive in the lungs for a long time, and will develop into (lung) metastases after rapid or slow oncogene activation, which suggests that cell proliferation and planting in other parts can be happened before the malignant change [26]. Recently, some scholars believe that the primary tumor is nourished by circulating tumor cells.
According to this "self-implantation", even in the early stages of tumorigenesis, a large number of tumor cells have appeared in the circulation, and were found far earlier than distant metastases [26]. Some research results have found that the regulation of the microenvironment before liver metastasis, such as the activation of various cells, the regulation of immune responses, and changes in cytokine levels, play a decisive role in the occurrence and development of liver metastases in digestive system tumors [27]. is an innovation in tumor treatment concepts and methods, and has great significance for the long-term survival of tumor patients [30].