A recent study shows that the global cancer burden is increasing (1). The research on the molecular mechanism and target of the occurrence and development of malignant tumors may be a breakthrough to solve this problem. Recently, it has been proved that TME is a key factor in the occurrence and development of malignant tumors, which is being the well-known hotspot. However, due to the influence of tumor cells and abnormal vascular structure, TME often shows the characteristics of hypoxia, especially in solid tumors.

Under the condition of hypoxia, the expression of HIF increases, and a series of changes have taken place in the metabolic mode and immune function of TME. In order to adapt to the influence of hypoxia, tumor cells have changed their metabolic mode and obtained energy through glycolysis. Meanwhile, immune cells are regulated by hypoxia and have different effects. Among them, the function of immune cells that play an anti-tumor role is inhibited, such as cytotoxic T cells, B cells, and natural killer (NK) cells. However, the expression of immunosuppressive cells such as marrow-derived suppressor cells (MDSC) and regulatory (Treg) T cells is up-regulated. The changes of metabolism and immune effect provide an excellent living environment for tumor cells and hinder the effect of anti-tumor treatment. In addition, while providing survival conditions for tumor cells, TME under hypoxia obstructs the effect of antitumor drugs by hindering drug delivery (2–4). Therefore, traditional chemotherapy and single dose immunotherapy cannot achieve satisfactory results, which makes the treatment of malignant tumors challenging (5, 6).

In conclusion, hypoxia, as an independent prognostic indicator related to poor survival rate of cancer patients, is expected to become an effective target for fighting tumor and alleviating drug resistance (7). After summarizing, we found that people are increasingly interested in the field of hypoxia in TME, and hundreds of relevant academic papers in this field have been published (8). Among the published studies, research targeting metabolic enzymes, HIF, and angiogenesis related factors have made breakthroughs to varying degrees. Currently, what’s exciting is more than 500 clinical trials have been adopt. In this review, we describe the effects of hypoxia on the proliferation, metastasis, and drug resistance of tumor cells in the TME from the perspectives of immunity, metabolism and HIF, and summarize the different treatment strategies targeting hypoxia. Finally, we summarized the current measures to combat drug resistance and the prospects for future research in this field.

TME is a cellular environment that harbors the tumor, composed of tumor cells, fibroblasts, immune cells (T cells, B cells, natural killer (NK) cells, and tumor-associated macrophages (TAMs)), blood vessels, signaling molecules, and extracellular matrix (9, 10). Hypoxia is ubiquitous property in the TME, especially in solid tumors. Abnormal blood vessels in the tumor tissue cannot meet the excessive oxygen and nutrient demand for its rapid growth, leading to uneven hypoxia. Thus, the area away from the blood vessels was anoxic, while the adjacent tumor tissue was hyper-oxygenated. A recent study suggested that hypoxia affects the immune microenvironment and makes tumor cells escape from immune monitoring and killing (11). As shown in Figure 1 , the anoxic area in tumor tissue hinders the infiltration of immune cells and promotes the growth of tumor cells (12).

Hypoxia affects the TME and alters the tumor and the surrounding tissue metabolism. With the progress of TME studies, metabolic reprogramming has been recognized as a hallmark behavior of malignant tumors. As shown in Figure 2 , metabolic reprogramming is the metabolic modification of tumor cells to maintain growth and resist treatment. This reprogramming includes aerobic glycolysis and L-glutamine metabolism et al (51). Thus, it could be deduced that hypoxia inhibits the apoptosis of tumor cells by promoting the metabolic reprogramming of tumor cells.

HIF is a major factor that mediates tumor cells to adapt to hypoxia (69). HIF-1α transcription factor directly targets VEGF, TGF-β, IL-10, and PD-L1 genes and regulates the tumor immunosuppressive response to CAFs (70–72). HIF is a heterodimer helical-loop protein consisting of an O₂-sensitive α-subunit (including HIF-1α, HIF-2α, and HIF-3α) and a constitutive β-subunit (16). HIF-1α plays a key role in several steps of hypoxia induction (73). In case of hypoxia, HIF-1α breakdown is reduced and transferred to the nucleus when the function of prolyl hydroxylase (PHD-RRB is inhibited. In the cell nucleus, HIF-1α binds to HIF-1β to form heterodimers. HIF-1α/1β heterodimer activates the HIF target gene and promotes HIF expression by combining the HIF-1α/1β heterodimer with p300/CBP and hypoxia response element (HRE), thus regulating various biological processes of tumor cells, including metabolic reprogramming, immunoregulation, angiogenesis, tumor cell invasion, and drug resistance (74, 75).

Among them, HIF could inhibit the immune response by promoting the up regulation of immune checkpoints, apoptosis of cytotoxic T cells and blocking phagocytosis, which is conducive to the occurrence and development of tumor cells. Studies have reported that the up-regulated immune checkpoint PD-L1 in tumor cells presents HIF-1α dependence, promote the apoptosis of cytotoxic T cells, and participate in the immune escape of tumor cells (76, 77). Similarly, the expression of CD47 protein on the surface of tumor cells is also affected by HIF-1α, and hinder the phagocytic ability of phagocytes to tumor cells through phosphorylation of signal regulatory proteins on the surface of macrophages α (SIRP α) (78). In recent years, the research results of CD47 protein showed that the expression of CD47 protein also inhibited the function of cytotoxic T cells and NK cells. Therefore, a series of clinical studies targeting CD47 protein are expected to bring new hope to the field of tumor therapy (79, 80). In addition, vascular endothelial growth factor (VEGF) is up-regulated affected by HIF-1α, which could promote metastasis and immune escape by inducing tumor angiogenesis. It is believed that the disorder of TGF-β is related to the occurrence and development of tumors, and enhances the invasive ability of tumor cells by inducing epithelial to mesenchymal transition (EMT) (81, 82). The research of Huang et al. showed that the HIF-1α regulate the function of TGF-β by forming Smad-HIF-1α complex under hypoxia, and then regulate the progress of tumor cells (83).

In addition to the inhibition of immune effects in TME, HIF-1 activates or inhibits the genes of key proteins in glycolysis pathway to regulate the metabolic process of tumor cells in hypoxic environment. Proteins or genes involved in the regulation of glycolysis pathway and regulated by HIF-1 include those involved in encoding glucose transporters (GLUT1 and GLUT3), hexokinases (HK1 and hK2), lactate dehydrogenase A (LDHA), etc (84–88). At the same time, oxidative phosphorylation related genes and proteins are negatively regulated by HIF-1. The differential regulation of proteins or genes relating glycolysis and oxidative phosphorylation by HIF-1 is conducive to the adaptation of tumor cells to achieve glucose metabolism reorganization. In addition, tumor cells reprogrammed by glucose metabolism have higher “competitiveness” to glucose in the microenvironment, so T cell apoptosis is induced by inhibition of energy metabolism, which aggravates the inhibition of T cell function. Except the glycolysis, HIF, as a major regulator, is involved in regulating glutamine metabolism in tumor cells (89). Under the condition of hypoxia, HIF-2α causes the change in SLC1A5 gene encoding neutral amino acid transporter, which mediates the reprogramming of glutamine metabolism and the resistance to gemcitabine in tumor cells (90). Moreover, HIF inhibit α- Ketoglutarate participates in the tricarboxylic acid cycle by promoting α- Ketoglutarate dehydrogenase (αKGDH) degradation (91). In addition, HIF is also involved in regulating many metabolic pathways, such as fatty acids, pentose phosphate and adenosine, so as to provide a metabolic basis for the progression and metastasis of tumor cells.

In summary, the important role of HIF in tumor progression and its potential mechanism have been widely concerned by researchers. Further research in this field in the future is expected to help us have a deeper understanding of hypoxic TME, and bring new hope to the research of tumor targeted therapy (92).

ROS are the main molecules produced by oxidative stress and have been considered major factors in the tumor occurrence, development, and recurrence. The ROS in tumor cells originate from mitochondria (93). Under the influence of hypoxia, the oxygen utilization efficiency of tumor cells is decreased. Therefore, electron transport efficiency through the mitochondrial complexes in the electron transport chain (ETC) is reduced, resulting in abundant ROS in cells (94, 95). Notably, various concentrations of ROS exert different effects on tumor cell production (96). High concentrations of ROS disrupt the proteins and nucleic acids and induce apoptosis of tumor cells through oxidative stress (97). A low concentration of ROS can promote the development and metastasis of tumor cells (98). In addition, the concentration of ROS affects the sensitivity and resistance of tumor cells to chemotherapeutic drugs, which might be related to the level of p-glycoprotein (P-gp) in drug resistance (99) ( Figure 2 ).

To date, chemotherapy is the cornerstone of cancer treatment. Anoxic metabolic disorders and changes in the microenvironment severely inhibit the efficacy of drugs such as Bleomycin. This could be because the oxygen-dependent chemotherapy drugs are more active when oxygen is available (100), while hypoxia directly inhibits the antitumor function of oxygen-dependent chemotherapeutic drugs (101). In addition, hypoxia indirectly reduces the efficacy of the drugs by interfering with the cell cycle, promoting DNA repair, and reducing the sensitivity of p53-mediated apoptosis (29, 102). Intriguingly, immunotherapy has developed rapidly in the past decade and has produced significant clinical results. However, the current studies have suggested that hypoxic stimulation significantly limits the effectiveness of immunotherapy (21, 103, 104). About 33% of patients who responded to immunotherapy suffered resistance again (6). Hypoxia effectuates metabolic changes in tumor cells, including low pH, high ROS, abnormal blood vessels, and proliferating fibrous tissue. These changes are beneficial to tumor cell survival, provide anti-apoptosis advantages, inhibit drug penetration, and promote the development of cancer and drug resistance (105).

To confront the challenge of drug resistance, the main methods include early diagnosis, combined multi drug therapy, and adaptive therapy (106). Effective evaluation molecules could provide a good reference for the early diagnosis and progress of malignant tumors. Quantitative monitoring of circulating tumor DNA (ctDNA) is expected to become an important means of early diagnosis and dynamic monitoring of cancer, which will help to improve the overall survival rate and guide individualized treatment (107). Combined with positron emission tomography and computed tomography (PET-CT) imaging results, evaluate the curative effect. And then adjust the drugs, so as to avoid the emergence of drug resistance and achieve better curative effect (108). Meanwhile, precise drug delivery methods such as antibody drug conjugate (ADC) could increase the curative effect by increasing the local drug concentration (109). In addition, multi drug combination therapy is still an effective measure to combat drug resistance at present. The research of Niu et al. shows that the combined application of vibostolimab (anti-TIGIT humanized IgG1 monoclonal antibody) and pembrolizumab can significantly inhibit and improve the drug resistance of non-small cell lung cancer (NSCLC) (110).

Bibliometric research published on Frontiers in oncology shows that researchers’ interest in the research of tumor microenvironment is continuously rising from 2011 to 2021 (8). Moreover, the current research hotspot in this field focuses on the energy metabolism, oxidative phosphorylation, liposomes and other new drug delivery routes in TME (8). Therefore, in order to facilitate readers to understand the progress in this field, we summarize the treatment strategies that targeted at hypoxia. It is gratifying that several potential anti-tumor targets have been found ( Table 1 ), including targeting hypoxia, glycolytic drugs, abnormal angiogenesis, and HIF drugs.

The energy metabolism of tumor microenvironment is a current research hotspot, and researchers have carried out a series of studies with it. A current study showed that glycolytic inhibitors effectively kill tumor cells that are not sensitive to chemotherapy drugs, even when they were present in multiple drug resistance cells (161, 162). Hexokinase 2 (HK2) plays a critical role in regulating aerobic glycolysis in tumor cells and has become one of the main targets of tumor therapy. A previous study showed that HK2 inhibitor 3-bromopyruvic acid (3-BP) significantly inhibits the progression and proliferation of tumor cells in HK2- expressing colorectal cancer. Moreover, apoptosis of tumor cells was induced by the signaling pathway of mitochondrial apoptosis (163). In recent years, the emergence of chemical dynamic therapy (CDT) has provided a new solution for cancer treatment (164). Interestingly, the amount of glutathione in the tumor cells directly affects the efficacy of chemotherapy. Glycolytic inhibitors could reduce the tumor’s glycolytic process and enhance CDT selectivity to tumor cells, thereby exploiting metabolic differences to achieve the specific treatment for tumor cells (165). In addition, OXPHOS inhibitors, such as metformin, improve hypoxia in the microenvironment by inhibiting the mitochondrial complex I, which reduces oxygen consumption in cells and corrects the hypoxic TME. Besides, OXPHOS also inhibits the upregulation of cancer subtypes, such as ovarian cancer, prostate cancer, and thyroid cancer (166, 167).

Abnormal tumor blood vessels are major factors in the continuous hypoxia of TME that hinder drug delivery (168). In the hypoxic TME, angiogenesis-promoting cytokines, such as VEGF and TGF-β, impede the differentiation and maturation of endothelial cells in neovascularization. As a result, malformed and poorly permeable new blood vessels aggravate the anoxic state of the tumor, making it difficult to deliver drugs effectively to the tumor (169). Antiangiogenic drugs, such as anti-VEGF antibodies, correct the abnormal blood vessels and promote the normalization of tumor blood vessels, which in turn alleviates hypoxia and improves the efficacy of conventional antitumor drugs (170, 171). However, angiogenesis inhibitors alone do not receive ideal therapeutic results, which might be related to the complex mechanisms of angiogenesis compensation (172). Therefore, VEGF inhibitors need to be used in combination with chemotherapy or immunotherapy, which has achieved satisfactory results in solid tumors, such as ovarian and breast cancer (173, 174).

HIF activity is mainly dependent on HIF-1α and plays a critical role in the regulation of hypoxic TME. Presently, studies on targeting HIF-1α are being widely carried out. Targeting the HIF-1α signaling pathway is effective in the treatment of solid tumors, such as pancreatic cancer (175, 176). Ubiquitin carboxy-terminal hydrolase L 1(UCHL1) is a ubiquitin-free enzyme that stabilizes its α-subunit (HIF-1α). UCHL1 inhibitors promote the degradation of HIF-1α and inhibit the activity of its downstream genes. Li et al. showed that the inhibition of the UCHL1-HIF-1 pathway decreases the expression of malignant tumor-related factors and eliminates UCHL1-mediated tumor cell proliferation and metastasis (177). In addition, Nelson et al. found that in the hypoxic microenvironment of pancreatic cancer, downregulation of USP25 reduced the transcriptional activity of HIF-1α, leading to cell death in the hypoxic core of the tumor without normal tissue affected (118). In another mouse model of pancreatic cancer, Xu et al. demonstrated that the Benzofuran derivative inhibited tumor growth by acting on the HIF-1α/VEGF pathway under hypoxia (111). In addition, the combination of the HIF-1α inhibitor px-478 and the immune-checkpoint inhibitor enhances the cytotoxicity of T cells against tumor cells, which might be related to the blocking of the HIF-1α/LOXL2 signaling pathway (178). Currently, clinical trials of combined therapy with HIF-1α inhibitors are underway. Thus, HIF-1α inhibitors seem to be a promising cancer therapy in the future.

Of note, the selective is not negligible for drug development, anoxic prodrug is an inactive compound that could be activated automatically in a specific anoxic region. This exploits the selective metabolism of precursor drugs in an anoxic environment, diffuses the killing compounds to the whole TME, and realizes the selective killing of tumor cells (179). A randomized controlled trial for the treatment of advanced pancreatic cancer showed that hypoxia-activated prodrug TH-302 combined with GissiTabine drug yields promising results; the combination group achieved more median progression-free survival than the single Gissi treatment group (180). In addition, TH-302 combined immune checkpoint blocking therapy cured >80% of the tumors in a mouse model of prostate cancer, which prolongs the suppression of bone MDSCs and relieves the inhibition of T cell proliferation (181). Another study showed that CP-506, an anoxic prodrug of nitrogen mustard, also yielded satisfactory effects in tumor tissue (182).

Hyperbaric medicine improves hypoxia in the TME by increasing the amount of dissolved oxygen in the blood (183). In previous studies, hyperbaric medicine has shown a satisfactory excellent curative effect in some cancers (breast and ovarian cancer) (184, 185). Hyperbaric oxygen (HBO) can be used as an adjuvant therapy to inhibit tumors by improving the hypoxic microenvironment (186). A recent study showed that hyperbaric medicine in mice with lung cancer improves the anoxic state of tumors, promotes tumor cell apoptosis, and inhibits tumor growth (187).

Hypoxia is the key factor regulating TME, which mediates the occurrence, development, and drug resistance of tumor cells. Under the condition of hypoxia, TME show immunosuppression and metabolic reprogramming. Therefore, the proliferation and differentiation of immune cells were inhibited. Immunosuppressive cells such as MDSCs, TAM and Tregs are recruited to the hypoxic zone to promote the escape of tumor cells. The metabolic reprogramming of tumor cells is conducive to obtaining energy in a hypoxic environment while maintaining an acidic microenvironment. In addition, glutamine metabolism and fatty acid metabolism have made great contributions to the balanced redox, anti-apoptosis, growth promotion and drug resistance of tumor cells. More importantly, while the hypoxia inhibits the function of PHD, HIF-1α will be activated and promotes the expression of downstream target genes, which further promotes the formation of hypoxic microenvironment and the progress of tumor cells. Therefore, anti-tumor therapy targeting hypoxia and related factors has attracted many researchers’ exploration. Finally, drug resistance induced by hypoxia still plays an important role in the process of anti-tumor treatment, which significantly affects the outcome of treatment. In this review, we summarize the treatment schemes for hypoxia, such as glycolysis inhibitors, anti-angiogenesis drugs, HIF inhibitors, hypoxia-activated prodrugs, and hyperbaric medicine, and finally the found targets and signal pathways in the form of table.

In conclusion, hypoxia is still the key to fight against malignant tumors. It is very necessary to clarify the molecular mechanism of hypoxia on the formation of tumor microenvironment and drug resistance, which will contribute to the breakthrough of tumor targeted therapy in the following work.

(I) Conception and design: TH, DX. (II) Searching literature and led the writing of the review: DX, GC. (III) Making figures and table: GC, KW, HL. (IV) Final approval of manuscript: All authors.

This work was supported in part by the Shanghai “Rising Stars of Medical Talent” Youth Development Program, Outstanding Youth Medical Talents.

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.