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In vitro assessment of a gallium-doped glass polyalkenoate cement: chemotherapeutic potential, cytotoxicity and osteogenic effects
Metastatic bone lesions are often osteolytic, which causes advanced-stage cancer sufferers to experience severe pain and an increased risk of developing a pathological fracture. Gallium (Ga) ion possesses antineoplastic and anti-bone resorption properties, suggesting the potential for its local admi...
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| Published in: | Biomedical materials (Bristol) 2024-09, Vol.19 (5), p.55006 |
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| container_issue | 5 |
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| container_title | Biomedical materials (Bristol) |
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| creator | Phull, Sunjeev Marx, Daniella Akens, Margarete K Ghert, Michelle Towler, Mark R |
| description | Metastatic bone lesions are often osteolytic, which causes advanced-stage cancer sufferers to experience severe pain and an increased risk of developing a pathological fracture. Gallium (Ga) ion possesses antineoplastic and anti-bone resorption properties, suggesting the potential for its local administration to impede the growth of metastatic bone lesions. This study investigated the chemotherapeutic potential, cytotoxicity, and osteogenic effects of a Ga-doped glass polyalkenoate cement (GPC) (C-TA2) compared to its non-gallium (C-TA0) counterpart. Ion release profiles revealed a biphasic pattern characterized by an initial burst followed by a gradually declining release of ions. C-TA2 continued to release Ga steadily throughout the experimentation period (7 days) and exhibited prolonged zinc (Zn) release compared to C-TA0. Interestingly, the Zn release from both GPCs appeared to cause a chemotherapeutic effect against H1092 lung cancer cells in vitro, with the prolonged Zn release from C-TA2 extending this effect. Unfortunately, both GPCs enhanced the viability of HCC2218 breast cancer cells, suggesting that the chemotherapeutic effects of Zn could be tied to cellular differences in preferred Zn concentrations. The utilization of SAOS-2 and MC3T3 cell lines as bone cell models yielded conflicting results, with the substantial decline in MC3T3 viability closely associated with silicon (Si) release, indicating cellular variations in Si toxicity. Despite this ambiguity, both GPCs exhibited harmful effects on the osteogenesis of primary rat osteoblasts, raising concerns about excessive burst Zn release. While Ga/Zn-doped GPCs hold promise for treating metastatic bone lesions caused by lung cancers, further optimization is required to mitigate cytotoxicity on healthy bone. |
| doi_str_mv | 10.1088/1748-605X/ad5ba5 |
| format | article |
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Unfortunately, both GPCs enhanced the viability of HCC2218 breast cancer cells, suggesting that the chemotherapeutic effects of Zn could be tied to cellular differences in preferred Zn concentrations. The utilization of SAOS-2 and MC3T3 cell lines as bone cell models yielded conflicting results, with the substantial decline in MC3T3 viability closely associated with silicon (Si) release, indicating cellular variations in Si toxicity. Despite this ambiguity, both GPCs exhibited harmful effects on the osteogenesis of primary rat osteoblasts, raising concerns about excessive burst Zn release. 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Interestingly, the Zn release from both GPCs appeared to cause a chemotherapeutic effect against H1092 lung cancer cells in vitro, with the prolonged Zn release from C-TA2 extending this effect. Unfortunately, both GPCs enhanced the viability of HCC2218 breast cancer cells, suggesting that the chemotherapeutic effects of Zn could be tied to cellular differences in preferred Zn concentrations. The utilization of SAOS-2 and MC3T3 cell lines as bone cell models yielded conflicting results, with the substantial decline in MC3T3 viability closely associated with silicon (Si) release, indicating cellular variations in Si toxicity. Despite this ambiguity, both GPCs exhibited harmful effects on the osteogenesis of primary rat osteoblasts, raising concerns about excessive burst Zn release. While Ga/Zn-doped GPCs hold promise for treating metastatic bone lesions caused by lung cancers, further optimization is required to mitigate cytotoxicity on healthy bone.</description><subject>bone metastasis</subject><subject>cancer</subject><subject>drug delivery</subject><subject>glass polyalkenoate cement</subject><issn>1748-6041</issn><issn>1748-605X</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2024</creationdate><recordtype>article</recordtype><recordid>eNp1kD1PwzAURS0EoqWwMyFvLA21mzix2VDFR6VKLCCxWS_Oc5uSxFHsIrryy0lV6ATTs94915YPIZec3XAm5YRniYxSJt4mUIgcxBEZHlbHh3PCB-TM-zVjQolYnZJBLBXP5JQNyde8oR9l6BwF79H7GptAnaVAl1BV5aaOCtdiQZdVn9PWVVuo3rFxEJAa3NG31KywdmGFHbS4CaXpsdAHJVRjarbBBfdZmjJsKTQFdT6gW2LTY2gtmuDPyYmFyuPFzxyR14f7l9lTtHh-nM_uFpGZpixEKoUMTJbGKgGrjLBZbjPLUAEkXCYCeCFEjCKRErIiTyERbCokTxmoaaZYPCJsf6_pnPcdWt12ZQ3dVnOmdzr1zpfeudN7nX3lal9pN3mNxaHw668HrvdA6Vq9dpuu6X-g87rWXGmhmRCMpbotbE-O_yD_ffkb0lCQCA</recordid><startdate>20240901</startdate><enddate>20240901</enddate><creator>Phull, Sunjeev</creator><creator>Marx, Daniella</creator><creator>Akens, Margarete K</creator><creator>Ghert, Michelle</creator><creator>Towler, Mark R</creator><general>IOP Publishing</general><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><orcidid>https://orcid.org/0000-0003-0752-6243</orcidid></search><sort><creationdate>20240901</creationdate><title>In vitro assessment of a gallium-doped glass polyalkenoate cement: chemotherapeutic potential, cytotoxicity and osteogenic effects</title><author>Phull, Sunjeev ; Marx, Daniella ; Akens, Margarete K ; Ghert, Michelle ; Towler, Mark R</author></sort><facets><frbrtype>5</frbrtype><frbrgroupid>cdi_FETCH-LOGICAL-c260t-96a7ac76394af9c5f7bf7f0e9aa41845a1d553e5488a7db6a450258160a927903</frbrgroupid><rsrctype>articles</rsrctype><prefilter>articles</prefilter><language>eng</language><creationdate>2024</creationdate><topic>bone metastasis</topic><topic>cancer</topic><topic>drug delivery</topic><topic>glass polyalkenoate cement</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Phull, Sunjeev</creatorcontrib><creatorcontrib>Marx, Daniella</creatorcontrib><creatorcontrib>Akens, Margarete K</creatorcontrib><creatorcontrib>Ghert, Michelle</creatorcontrib><creatorcontrib>Towler, Mark R</creatorcontrib><collection>PubMed</collection><collection>CrossRef</collection><jtitle>Biomedical materials (Bristol)</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Phull, Sunjeev</au><au>Marx, Daniella</au><au>Akens, Margarete K</au><au>Ghert, Michelle</au><au>Towler, Mark R</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>In vitro assessment of a gallium-doped glass polyalkenoate cement: chemotherapeutic potential, cytotoxicity and osteogenic effects</atitle><jtitle>Biomedical materials (Bristol)</jtitle><stitle>BMM</stitle><addtitle>Biomed. Mater</addtitle><date>2024-09-01</date><risdate>2024</risdate><volume>19</volume><issue>5</issue><spage>55006</spage><pages>55006-</pages><issn>1748-6041</issn><eissn>1748-605X</eissn><coden>BMBUCS</coden><abstract>Metastatic bone lesions are often osteolytic, which causes advanced-stage cancer sufferers to experience severe pain and an increased risk of developing a pathological fracture. Gallium (Ga) ion possesses antineoplastic and anti-bone resorption properties, suggesting the potential for its local administration to impede the growth of metastatic bone lesions. This study investigated the chemotherapeutic potential, cytotoxicity, and osteogenic effects of a Ga-doped glass polyalkenoate cement (GPC) (C-TA2) compared to its non-gallium (C-TA0) counterpart. Ion release profiles revealed a biphasic pattern characterized by an initial burst followed by a gradually declining release of ions. C-TA2 continued to release Ga steadily throughout the experimentation period (7 days) and exhibited prolonged zinc (Zn) release compared to C-TA0. Interestingly, the Zn release from both GPCs appeared to cause a chemotherapeutic effect against H1092 lung cancer cells in vitro, with the prolonged Zn release from C-TA2 extending this effect. Unfortunately, both GPCs enhanced the viability of HCC2218 breast cancer cells, suggesting that the chemotherapeutic effects of Zn could be tied to cellular differences in preferred Zn concentrations. The utilization of SAOS-2 and MC3T3 cell lines as bone cell models yielded conflicting results, with the substantial decline in MC3T3 viability closely associated with silicon (Si) release, indicating cellular variations in Si toxicity. Despite this ambiguity, both GPCs exhibited harmful effects on the osteogenesis of primary rat osteoblasts, raising concerns about excessive burst Zn release. 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| source | Institute of Physics:Jisc Collections:IOP Publishing Read and Publish 2024-2025 (Reading List) |
| subjects | bone metastasis cancer drug delivery glass polyalkenoate cement |
| title | In vitro assessment of a gallium-doped glass polyalkenoate cement: chemotherapeutic potential, cytotoxicity and osteogenic effects |
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