Expression of Hypoxia-Inducible Cell-Surface Transmembrane Carbonic Anhydrases in Human Cancer
Sergey Ivanov,Shu-Yuan Liao,Alla V. Ivanova,Alla Danilkovitch-Miagkova,Nadezhda Tarasova,Gregor Weirich,Marsha J. Merrill,Martin A. Proescholdt,Edward H. Oldfield,Joshua D. Lee,Jan Zavada,Abdul Waheed,William S. Sly,Michael I. Lerman,Eric J. Stanbridge +14 more
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TLDR
The studies show an important causal link between hypoxia, extracellular acidification, and induction or enhanced expression of these enzymes in human tumors and conclude that the cell surface transmembrane carbonic anhydrases CA IX and CA XII are overexpressed in many tumors suggesting that this is a common feature of cancer cells that may be required for tumor progression.Abstract:
An acidic extracellular pH is a fundamental property of the malignant phenotype. In von Hippel-Lindau (VHL)-defective tumors the cell surface transmembrane carbonic anhydrase (CA) CA9 and CA12 genes are overexpressed because of the absence of pVHL. We hypothesized that these enzymes might be involved in maintaining the extracellular acidic pH in tumors, thereby providing a conducive environment for tumor growth and spread. Using Northern blot analysis and immunostaining with specific antibodies we analyzed the expression of CA9 and CA12 genes and their products in a large sample of cancer cell lines, fresh and archival tumor specimens, and normal human tissues. Expression was also analyzed in cultured cells under hypoxic conditions. Expression of CA IX and CA XII in normal adult tissues was detected only in highly specialized cells and for most tissues their expression did not overlap. Analysis of RNA samples isolated from 87 cancer cell lines and 18 tumors revealed high-to-moderate levels of expression of CA9 and CA12 in multiple cancers. Immunohistochemistry revealed high-to-moderate expression of these enzymes in various normal tissues and multiple common epithelial tumor types. The immunostaining was seen predominantly on the cell surface membrane. The expression of both genes was markedly induced under hypoxic conditions in tumors and cultured tumor cells. We conclude that the cell surface trans-membrane carbonic anhydrases CA IX and CA XII are overexpressed in many tumors suggesting that this is a common feature of cancer cells that may be required for tumor progression. These enzymes may contribute to the tumor microenvironment by maintaining extracellular acidic pH and helping cancer cells grow and metastasize. Our studies show an important causal link between hypoxia, extracellular acidification, and induction or enhanced expression of these enzymes in human tumors.read more
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Acidity generated by the tumor microenvironment drives local invasion
Veronica Estrella,Tingan Chen,Mark C. Lloyd,Jonathan W. Wojtkowiak,Heather H. Cornnell,Arig Ibrahim-Hashim,Kate M. Bailey,Yoganand Balagurunathan,Jennifer M. Rothberg,Bonnie F. Sloane,Joseph O. Johnson,Robert A. Gatenby,Robert J. Gillies +12 more
TL;DR: Oral administration of sodium bicarbonate was sufficient to increase peritumoral pH and inhibit tumor growth and local invasion in a preclinical model, supporting the acid-mediated invasion hypothesis.
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TL;DR: Although now recognized as a major contributor to cancer progression and to treatment failure, the precise role of hypoxia signalling in cancer and in prognosis still needs to be further defined.
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Estrogen Receptor Status in Breast Cancer Is Associated with Remarkably Distinct Gene Expression Patterns
Sofia Gruvberger,Markus Ringnér,Yi Chen,Sujatha Panavally,Lao H. Saal,Åke Borg,Mårten Fernö,Carsten Peterson,Paul S. Meltzer +8 more
TL;DR: The results provide evidence that ER+ and ER- tumors display remarkably different gene-expression phenotypes not solely explained by differences in estrogen responsiveness, and could accurately predict ER status even when excluding top discriminator genes, including ER itself.
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Hypoxia-Inducible Carbonic Anhydrase IX and XII Promote Tumor Cell Growth by Counteracting Acidosis through the Regulation of the Intracellular pH
Johanna Chiche,Karine Ilc,Julie Laferrière,Eric Trottier,Frédéric Dayan,Nathalie M. Mazure,M. Christiane Brahimi-Horn,Jacques Pouysségur +7 more
TL;DR: Hypoxia-induced CAIX and CAXII are major tumor prosurvival pH(i)-regulating enzymes, and their combined targeting shows that they hold potential as anticancer targets.
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Carbonic anhydrase IX is an independent predictor of survival in advanced renal clear cell carcinoma: Implications for prognosis and therapy
Matthew H. T. Bui,David Seligson,Ken Ryu Han,Allan J. Pantuck,Frederick J. Dorey,Yunda Huang,Steve Horvath,Bradley C. Leibovich,Shefali Chopra,Shu Yuan Liao,Eric J. Stanbridge,Michael I. Lerman,Aarno Palotie,Robert A. Figlin,Arie S. Belldegrun +14 more
TL;DR: Lower CAIX levels are independently associated with poor survival in advanced RCC, which reflects significant changes in tumor biology, which should be used to predict clinical outcome and identify high-risk patients in need for adjuvant immunotherapy and CAIX-targeted therapies.
References
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Patterns and Emerging Mechanisms of the Angiogenic Switch during Tumorigenesis
TL;DR: The work from the authors' laboratories reviewed herein was supported by grants from the National Cancer Institute.
Journal ArticleDOI
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Journal ArticleDOI
Openings between Defective Endothelial Cells Explain Tumor Vessel Leakiness
Hiroya Hashizume,Peter Baluk,Shunichi Morikawa,John W. McLean,Gavin Thurston,Sylvie Roberge,Rakesh K. Jain,Donald M. McDonald +7 more
TL;DR: It is concluded that some tumor vessels have a defective cellular lining composed of disorganized, loosely connected, branched, overlapping or sprouting endothelial cells that contribute to tumor vessel leakiness and may permit access of macromolecular therapeutic agents to tumor cells.
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Interstitial pH and pO2 gradients in solid tumors in vivo: high-resolution measurements reveal a lack of correlation.
TL;DR: The first combined, high-resolution measurements of interstitial pH and pO2 profiles between adjacent vessels in a human tumor xenograft are reported, using fluorescence ratio imaging and phosphorescence quenching microscopy.