Abstract
BackgroundThe Src tyrosine kinase phosphorylates effector proteins to induce expression of the podoplanin (PDPN) receptor in order to promote tumor progression. However, nontransformed cells can normalize the growth and morphology of neighboring transformed cells. Transformed cells must escape this process, called “contact normalization”, to become invasive and malignant. Contact normalization requires junctional communication between transformed and nontransformed cells. However, specific junctions that mediate this process have not been defined. This study aimed to identify junctional proteins required for contact normalization.MethodsSrc transformed cells and oral squamous cell carcinoma cells were cultured with nontransformed cells. Formation of heterocellular adherens junctions between transformed and nontransformed cells was visualized by fluorescent microscopy. CRISPR technology was used to produce cadherin deficient and cadherin competent nontransformed cells to determine the requirement for adherens junctions during contact normalization. Contact normalization of transformed cells cultured with cadherin deficient or cadherin competent nontransformed cells was analyzed by growth assays, immunofluorescence, western blotting, and RNA-seq. In addition, Src transformed cells expressing PDPN under a constitutively active exogenous promoter were used to examine the ability of PDPN to override contact normalization.ResultsWe found that N-cadherin (N-Cdh) appeared to mediate contact normalization. Cadherin competent cells that expressed N-Cdh inhibited the growth of neighboring transformed cells in culture, while cadherin deficient cells failed to inhibit the growth of these cells. Results from RNA-seq analysis indicate that about 10% of the transcripts affected by contact normalization relied on cadherin mediated communication, and this set of genes includes PDPN. In contrast, cadherin deficient cells failed to inhibit PDPN expression or normalize the growth of adjacent transformed cells. These data indicate that nontransformed cells formed heterocellular cadherin junctions to inhibit PDPN expression in adjacent transformed cells. Moreover, we found that PDPN enabled transformed cells to override the effects of contact normalization in the face of continued N-Cdh expression. Cadherin competent cells failed to normalize the growth of transformed cells expressing PDPN under a constitutively active exogenous promoter.ConclusionsNontransformed cells form cadherin junctions with adjacent transformed cells to decrease PDPN expression in order to inhibit tumor cell proliferation.Plain English SummaryCancer begins when a single cell acquires changes that enables them to form tumors. During these beginning stages of cancer development, normal cells surround and directly contact the cancer cell to prevent tumor formation and inhibit cancer progression. This process is called contact normalization. Cancer cells must break free from contact normalization to progress into a malignant cancer. Contact normalization is a widespread and powerful process; however, not much is known about the mechanisms involved in this process. This work identifies proteins required to form contacts between normal cells and cancer cells, and explores pathways by which cancer cells override contact normalization to progress into malignant cancers.Graphical abstract1_HLfVkYUa-1fjeHgGEFH3Video
Highlights
The Src tyrosine kinase phosphorylates effector proteins to induce expression of the podoplanin (PDPN) receptor in order to promote tumor progression
RNA-seq analysis was performed on Src transformed (MEC-Src) cells cultured with themselves, nontransformed (MEC) cells, and cadherin deficient (MEC-CdhKo) cells in the layered culture system. a A total of 49,315 unique gene transcripts were detected, with 21,738 expressed at a level of at least 1 transcript per million (TPM) in any of the cell types. b Analysis of transcripts from nontransformed (MEC) and Src transformed (MEC-Src) cells cultured with themselves indicate that oncogenic Src kinase altered the expression of 3391 transcripts by at least threefold (p < 0.05 by t-test, n = 3)
Contact normalization increased the expression of 326 genes that were originally inhibited by Src, and decreased the expression of 328 genes that were originally increased by Src. d Transcripts from Src transformed (MEC-Src) cells cultured with nontransformed (MEC) cells were compared with transcripts from mouse embryonic cells (MECs)-Src cells cultured with cadherin deficient (MEC-CdhKo) to identify genes affected by contact normalization in a cadherin dependent manner
Summary
The Src tyrosine kinase phosphorylates effector proteins to induce expression of the podoplanin (PDPN) receptor in order to promote tumor progression. Elucidating effects of oncogenic protein kinase activity on cell growth is a relatively direct task in cultured cell lines Results from these studies indicate that Src and other tyrosine kinases phosphorylate effectors including the Crk associated substrate/breast cancer antiestrogen resistance protein 1 (p130Cas/BCAR1) adaptor protein to induce expression of the podoplanin (PDPN) receptor in order to promote transformed cell growth and expansion [1,2,3,4,5]. Nontransformed cells can normalize the growth and morphology of neighboring transformed cells This process, called “contact normalization”, can control the growth of cells transformed by chemical carcinogens and oncogenic kinases including Src [6,7,8,9]. Contact normalization controls cell behavior downstream of Src kinase activity to inhibit expression of effectors including PDPN [4, 5, 10,11,12]
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
