Therapeutic potential of hyaluronan oligosaccharides for bone metastasis of breast cancer

Urakawa, Hiroshi; Nishida, Yoshihiro; Knudson, Warren; Knudson, Cheryl B.; Arai, Eisuke; Kozawa, Eiji; Futamura, Naohisa; Wasa, Junji; Ishiguro, Naoki

doi:10.1002/jor.21557

Cited by 44 publications

(46 citation statements)

References 43 publications

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“…In addition, 4-MU treatment inhibits a variety of HA signaling events, including downregulation of phospho-ErbB2, phospho-Akt, and downstream effectors MMP-2/MMP-9 and IL-8 expression (Fig. 2.1; Lokeshwar et al, 2010; Okuda et al, 2012; Twarock et al, 2011; Urakawa, Nishida, Wasa, et al, 2012). The efficacy of 4-MU as a glucuronate scavenger could contribute to its antitumor effects.…”

Section: Targeting Ha Productionmentioning

confidence: 99%

“…At concentrations of 0.2–1 mM (i.e., ~35–180 μg/ml), 4-MU inhibits proliferation, motility, and invasion, and causes loss of filopodia and focal adhesions, in a variety of cultured tumor cells (Arai et al, 2011; Hiraga, Ito, & Nakamura, 2013; Lokeshwar et al, 2010; Okuda et al, 2012; Piccioni et al, 2012; Twarock et al, 2011; Uchakina, Ban, & McKallip, 2013; Urakawa et al, 2012). 4-MU inhibits tumor spheroids and osteoclast-like cell formation (Hiraga et al, 2013) and downregulates the expression of both CD44 and RHAMM, suggesting a feedback loop between HA synthesis and HA receptor expression (Lokeshwar et al, 2010).…”

Section: Targeting Ha Productionmentioning

confidence: 99%

“…Nevertheless, at the concentrations used in cancer cells and tumor models and also the doses at which it is consumed as a dietary supplement, 4-MU is demonstrated to have antitumor activities. For example, in xenograft studies, oral administration of 4-MU has been shown to inhibit tumor growth and metastasis in prostate, B16 melanoma, skin, liver, osteosarcoma, breast, and esophageal cancer model systems (Bhattacharyya et al, 2009; Kudo et al, 2004; Lokeshwar et al, 2010; Nakazawa et al, 2006; Piccioni et al, 2012; Twarock et al, 2011; Urakawa, Nishida, Wasa, et al, 2012; Yoshihara et al, 2005). Recently, 4-MU was shown to inhibit bone metastasis in a breast cancer model (Hiraga et al, 2013).…”

Section: Targeting Ha Productionmentioning

confidence: 99%

“…Recently, 4-MU was shown to inhibit bone metastasis in a breast cancer model (Hiraga et al, 2013). As in the case of in vitro studies, some mouse xenograft studies have used 4-MU orally at doses as high as 1–3 g/kg; however, in other studies, 4-MU has shown remarkable efficacy at 200–400 mg/kg doses (Arai et al, 2011; Bhattacharyya et al, 2009; Hiraga et al, 2013; Kudo et al, 2004; Nakazawa et al, 2006; Okuda et al, 2012; Piccioni et al, 2012; Twarock et al, 2011; Urakawa, Nishida, Wasa, et al, 2012; Yoshihara et al, 2005). Based on the FDA’s formula of mouse-to-human dose conversion, 200–400 mg/kg doses in mice equates to 1.1–2.2 g/day doses in humans; these are doses at which 4-MU is consumed for improving liver health (Abate et al, 2001; Camarri & Marchettini, 1988; Garrett et al, 1993; Hoffmann et al, 2005; Quaranta et al, 1984; U.S.…”

Section: Targeting Ha Productionmentioning

confidence: 99%

“…Angiogenic HA fragments have been detected in the urine of patients with bladder cancer and Wilm’s tumor, in the saliva of patients with head and neck cancer, and in bladder and prostate tumor tissues (Franzmann et al, 2003; Kumar, West, Ponting, & Gattamaneni, 1989; Lokeshwar, Obek, Soloway, & Block, 1997; Lokeshwar et al, 2001). In contrast to the angiogenic HA fragments, HA oligosaccharides consisting of 2–3 disaccharide units have been shown to have antitumor activity, presumably because they inhibit HA-induced signaling (Ghatak, Misra, & Toole, 2002; Hosono et al, 2007; Toole, Ghatak, & Misra, 2008; Urakawa et al, 2012). …”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Targeting Hyaluronic Acid Family for Cancer Chemoprevention and Therapy

Lokeshwar

Mirza

Jordan

2014

Advances in Cancer Research

135

113

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Hyaluronic acid or hyaluronan (HA) is perhaps one of the most uncomplicated large polymers that regulates several normal physiological processes and, at the same time, contributes to the manifestation of a variety of chronic and acute diseases, including cancer. Members of the HA signaling pathway (HA synthases, HA receptors, and HYAL-1 hyaluronidase) have been experimentally shown to promote tumor growth, metastasis, and angiogenesis, and hence each of them is a potential target for cancer therapy. Furthermore, as these members are also overexpressed in a variety of carcinomas, targeting of the HA family is clinically relevant. A variety of targeted approaches have been developed to target various HA family members, including small-molecule inhibitors and antibody and vaccine therapies. These treatment approaches inhibit HA-mediated intracellular signaling that promotes tumor cell proliferation, motility, and invasion, as well as induction of endothelial cell functions. Being nontoxic, nonimmunogenic, and versatile for modifications, HA has been used in nanoparticle preparations for the targeted delivery of chemotherapy drugs and other anticancer compounds to tumor cells through interaction with cell-surface HA receptors. This review discusses basic and clinical translational aspects of targeting each HA family member and respective treatment approaches that have been described in the literature.

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Section: Targeting Ha Productionmentioning

confidence: 99%

Section: Targeting Ha Productionmentioning

confidence: 99%

Section: Targeting Ha Productionmentioning

confidence: 99%

Section: Targeting Ha Productionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Targeting Hyaluronic Acid Family for Cancer Chemoprevention and Therapy

Lokeshwar

Mirza

Jordan

2014

Advances in Cancer Research

135

113

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Targeting Signaling Pathways of Hyaluronic Acid and Integrin Receptors by Synergistic Combination Nanocomposites Inhibits Systemic Metastases and Primary Triple Negative Breast Cancer

Zhang

Alradwan

et al. 2021

Advanced Therapeutics

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Triple negative breast cancer (TNBC) has a poor prognosis due to its aggressive nature, high incidence of distant metastasis, and lack of targets for effective therapy. Therefore, a novel multifunctional biopolymer‐anticancer drug combination nanomedicine is designed for the prevention of spontaneous metastasis while treating primary TNBC. Oligomeric hyaluronic acid (oHA) and doxorubicin (DOX) at a synergistic ratio against TNBC cells are co‐loaded in a polymer‐lipid hybrid nanoparticle (PLN) which is then functionalized with an internalizing cyclic peptide iRGD (iRGD‐DOX‐oHA‐PLN). iRGD conjugation enhances cellular uptake and cytotoxicity in vitro and nanoparticle (NP) accumulation in human TNBC tumors that overexpress integrins. NP‐delivered oHA inhibits cell migration and invasion in vitro via the intracellular release of oHA that interacts with the receptor for hyaluronan mediated motility and downregulates the phospho‐extracellular signal‐regulated kinase (p‐ERK) signaling pathway. Intravenously injected iRGD‐DOX‐oHA‐PLN significantly inhibits the growth of primary TNBC tumors in a mouse model and prevents spontaneous metastasis to the lungs and lymph nodes, superior to free solutions of DOX, oHA, or both and NP formulations loaded with DOX or oHA. These results suggest that iRGD‐DOX‐oHA‐PLN can be a promising bioactive polymer‐drug combination nanomedicine for the treatment of TNBC and prevention of its spontaneous metastasis.

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The CD147‐HYALURONAN Axis in Cancer

Toole

2019

The Anatomical Record

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CD147 (basigin; EMMPRIN), hyaluronan, and hyaluronan receptors (e.g., CD44) are intimately involved in several phenomena that underlie malignancy. A major avenue whereby they influence tumor progression is most likely their role in the characteristics of cancer stem cells (CSCs), subpopulations of tumor cells that exhibit chemoresistance, invasiveness, and potent tumorigenicity. Both CD147 and hyaluronan have been strongly implicated in chemoresistance and invasiveness, and may be drivers of CSC characteristics, since current evidence indicates that both are involved in epithelial-mesenchymal transition, a crucial process in the acquisition of CSC properties. Hyaluronan is a prominent constituent of the tumor microenvironment whose interactions with cell surface receptors influence several signaling pathways that lead to chemoresistance and invasiveness. CD147 is an integral plasma membrane glycoprotein of the Ig superfamily and cofactor in assembly and activity of monocarboxylate transporters (MCTs). CD147 stimulates hyaluronan synthesis and interaction of hyaluronan with its receptors, in particular CD44 and LYVE-1, which in turn result in activation of multiprotein complexes containing members of the membrane-type matrix metalloproteinase, receptor tyrosine kinase, ABC drug transporter, or MCT families within lipid raft domains. Multivalent hyaluronan-receptor interactions are essential for formation or stabilization of these lipid raft complexes and for downstream signaling pathways or transporter activities. We conclude that stimulation of hyaluronan-receptor interactions by CD147 and the consequent activities of these complexes may be critical to the properties of CSCs and their role in malignancy. Anat Rec, 303:1573Rec, 303: -1583Rec, 303: , 2020

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Therapeutic potential of hyaluronan oligosaccharides for bone metastasis of breast cancer

Cited by 44 publications

References 43 publications

Targeting Hyaluronic Acid Family for Cancer Chemoprevention and Therapy

Targeting Hyaluronic Acid Family for Cancer Chemoprevention and Therapy

Targeting Signaling Pathways of Hyaluronic Acid and Integrin Receptors by Synergistic Combination Nanocomposites Inhibits Systemic Metastases and Primary Triple Negative Breast Cancer

The CD147‐HYALURONAN Axis in Cancer

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