Your search keyword '"Liu, Kela"' showing total 7 results

1. C4ST-1/CHST11-controlled chondroitin sulfation interferes with oncogenic HRAS signaling in Costello syndrome.

Author

Klüppel, Michael, Samavarchi-Tehrani, Payman, Liu, Kela, Wrana, Jeffrey L, and Hinek, Aleksander

Subjects

*CHONDROITIN sulfates, *COSTELLO syndrome, *GENETIC disorders in children, *SULFOTRANSFERASES, *SULFATION

Abstract

Costello syndrome is a pediatric genetic disorder linked to oncogenic germline mutations in the HRAS gene. The disease is characterized by multiple developmental abnormalities, as well as predisposition to malignancies. Our recent observation that heart tissue from patients with Costello syndrome showed a loss of the glycosaminoglycan chondroitin-4-sulfate (C4S) inspired our present study aimed to explore a functional involvement of the chondroitin sulfate (CS) biosynthesis gene Carbohydrate sulfotransferase 11/Chondroitin-4-sulfotransferase-1 (CHST11/C4ST-1), as well as an impaired chondroitin sulfation balance, as a downstream mediator of oncogenic HRAS in Costello syndrome. Here we demonstrate a loss of C4S, as well as a reduction in C4ST-1 mRNA and protein expression, in primary fibroblasts from Costello syndrome patients. We go on to show that expression of oncogenic HRAS in normal fibroblasts can repress C4ST-1 expression, whereas interference with oncogenic HRAS signaling in Costello syndrome fibroblasts elevated C4ST-1 expression, thus identifying C4ST-1 as a negatively regulated target gene of HRAS signaling. Importantly, we show that forced expression of C4ST-1 in Costello fibroblasts could rescue the proliferation and elastogenesis defects associated with oncogenic HRAS signaling in these cells. Our results indicate reduced C4ST-1 expression and chondroitin sulfation imbalance mediating the effects of oncogenic HRAS signaling in the pathogenesis of Costello syndrome. Thus, our work identifies C4ST-1-dependent chondroitin sulfation as a downstream vulnerability in oncogenic RAS signaling, which might be pharmacologically exploited in future treatments of not only Costello syndrome and other RASopathies, but also human cancers associated with activating RAS mutations. [ABSTRACT FROM AUTHOR]

Published

2012

2. Ellagic and Tannic Acids Protect Newly Synthesized Elastic Fibers from Premature Enzymatic Degradation in Dermal Fibroblast Cultures.

Author

Jimenez, Felipe, Mitts, Thomas F., Liu, Kela, Wang, Yanting, and Hinek, Aleksander

Subjects

*TANNINS, *FIBROBLASTS, *ELASTIN, *EXTRACELLULAR matrix proteins, *SKIN biopsy, *POLYPHENOLS, *MESSENGER RNA, *METALLOPROTEINASES

Abstract

Progressive proteolytic degradation of cutaneous elastic fibers, that cannot be adequately replaced or repaired by adult dermal fibroblasts, constitutes a major feature of aging skin. Our present investigations, employing monolayer cultures of human dermal fibroblasts and organ cultures of skin biopsies, were aimed at testing whether the hydrophilic tannic acid (TA) and lipophilic ellagic acid (EA) would protect dermal elastin from exogenous and endogenous enzymatic degradation. Results from both culture systems indicated that dermal fibroblasts, maintained with TA or EA, deposit significantly more elastic fibers than untreated control cultures despite the fact that neither polyphenol enhanced transcription of elastin mRNA or cellular proliferation. Results of a pulse and chase experiment showed that pretreatment with both polyphenols enhanced biostability of tropoelastin and newly deposited elastin. Results of in vitro assays indicated that both polyphenols bound to purified elastin and significantly decreased its proteolytic degradation by elastolytic enzymes belonging to the serine proteinase, cysteine proteinase, and metallo-proteinase families. Importantly, both polyphenols also synergistically enhanced elastogenesis induced by selected elastogenic compounds in cultures of dermal fibroblasts. We propose that EA and TA may be useful for preventing proteolytic degradation of existing dermal elastic fibers and for enhancing more efficient elastogenesis in aged skin.Journal of Investigative Dermatology (2006) 126, 1272–1280. doi:10.1038/sj.jid.5700285; published online 6 April 2006 [ABSTRACT FROM AUTHOR]

Published

2006

3. Proteolytic digest derived from bovine Ligamentum Nuchae stimulates deposition of new elastin-enriched matrix in cultures and transplants of human dermal fibroblasts

Author

Hinek, Aleksander, Wang, Yanting, Liu, Kela, Mitts, Thomas F., and Jimenez, Felipe

Subjects

*EXTRACELLULAR matrix proteins, *GLYCOPROTEINS, *FIBROBLASTS, *HYALURONIC acid

Abstract

Abstract: Background:: Diverse topical products and injectable fillers used for correcting facial wrinkles induce rather short-lived effects because they target replacement of dermal collagen and hyaluronan, matrix components of limited biologic durability. Objective:: Present studies were aimed at stimulation of fully differentiated human dermal fibroblasts to resume deposition of new extracellular matrix rich of elastin, the most durable and metabolically inert component of dermal ECM. Methods:: We have created a novel proteolytic digest of bovine ligamentum nuchae (ProK-60), and tested its potential biological effect on dermal fibroblasts derived from females of different ages. Northern blots, quantitative immunohistochemistry and metabolic assays were used to assess effects of ProK-60 on proliferation and matrix production in primary cultures of dermal fibroblasts, in cultures of skin explants and after implantation of stimulated fibroblasts into the skin of athymic nude mice. Results:: ProK-60 increased proliferation (25–30%) of cultured dermal fibroblasts and significantly enhanced their production of new elastic fibers (>250%) and collagen fibers (100%). These effects were mostly mediated by stimulation of cellular elastin receptor. In contrast, ProK-60 inhibited production of fibronectin (−30%) and chondroitin sulfate proteoglycans (−50%). ProK-60 also activated proliferation of dermal fibroblasts, mostly derived from the stratum basale and induced deposition of elastic fibers in cultures of skin explants. Moreover, human fibroblasts pre-treated with ProK-60 produced abundant elastic fibers after their injection into the skin of athymic nude mice. Conclusion:: The described biological effects of ProK-60, including its unique elastogenic property, encourage use of this compound in cosmetic formulations stimulating rejuvenation of aged skin. [Copyright &y& Elsevier]

Published

2005

4. Targeting tumour-associated macrophages in hodgkin lymphoma using engineered extracellular matrix-mimicking cryogels.

Author

Bahlmann, Laura C., Xue, Chang, Chin, Allysia A., Skirzynska, Arianna, Lu, Joy, Thériault, Brigitte, Uehling, David, Yerofeyeva, Yulia, Peters, Rachel, Liu, Kela, Chen, Jianan, Martel, Anne L., Yaffe, Martin, Al-awar, Rima, Goswami, Rashmi S., Ylanko, Jarkko, Andrews, David W., Kuruvilla, John, Laister, Rob C., and Shoichet, Molly S.

Subjects

*HODGKIN'S disease, *MITOGEN-activated protein kinases, *MACROPHAGES, *GLYCOSAMINOGLYCANS, *EXTRACELLULAR matrix, *DRUG target, *COLLAGEN

Abstract

Tumour-associated macrophages are linked with poor prognosis and resistance to therapy in Hodgkin lymphoma; however, there are no suitable preclinical models to identify macrophage-targeting therapeutics. We used primary human tumours to guide the development of a mimetic cryogel, wherein Hodgkin (but not Non-Hodgkin) lymphoma cells promoted primary human macrophage invasion. In an invasion inhibitor screen, we identified five drug hits that significantly reduced tumour-associated macrophage invasion: marimastat, batimastat, AS1517499, ruxolitinib, and PD-169316. Importantly, ruxolitinib has demonstrated recent success in Hodgkin lymphoma clinical trials. Both ruxolitinib and PD-169316 (a p38 mitogen-activated protein kinase (p38 MAPK) inhibitor) decreased the percent of M2-like macrophages; however, only PD-169316 enhanced the percentage of M1-like macrophages. We validated p38 MAPK as an anti-invasion drug target with five additional drugs using a high-content imaging platform. With our biomimetic cryogel, we modeled macrophage invasion in Hodgkin lymphoma and then used it for target discovery and drug screening, ultimately identifying potential future therapeutics. • Hodgkin lymphoma cells promote macrophage invasion and an M2-like phenotype. • JAK1/2 inhibitor ruxolitinib decreases Hodgkin lymphoma cell-induced macrophage invasion. • p38 MAPK is identified as a novel target against Hodgkin lymphoma-induced macrophage invasion. • p38 MAPK inhibitor PD-169316 repolarizes macrophages toward an M1-like phenotype. • Hodgkin lymphoma subtype dictates extracellular matrix composition of collagens, fibronectin, and glycosaminoglycans. [ABSTRACT FROM AUTHOR]

Published

2023

5. Whole-mount pathology of breast lumpectomy specimens improves detection of tumour margins and focality.

Author

Clarke, Gina M, Holloway, Claire M B, Zubovits, Judit T, Nofech‐Mozes, Sharon, Liu, Kela, Murray, Mayan, Wang, Dan, and Yaffe, Martin J

Subjects

*LUMPECTOMY, *BREAST cancer diagnosis, *BREAST cancer treatment, *BREAST surgery, *CHI-squared test, *SIMULATION methods & models

Abstract

Aims Technical limitations in conventional pathological evaluation of breast lumpectomy specimens may reduce diagnostic accuracy in the assessment of margin and focality. A novel technique based on whole-mount serial sections enhances sampling while preserving specimen conformation and orientation. The aim of this study was to investigate assessment of focality and margin status by the use of whole-mount serial sections versus simulated conventional sections in lumpectomies. Methods and results Two pathologists interpreted whole-mount serial sections and simulated conventional sections for 58 lumpectomy specimens by reporting the closest margin and focality. Measurements were compared by the use of McNemar's chi-squared test. Statistically significant differences were observed in the assignment of both margin positivity ( P = 0.014) and multifocality ( P = 0.021). A positive margin or multifocal disease was identified by the use of whole-mount serial sections but missed in the simulated conventional assessment in 10.3% and 17.2% of all cases, respectively. There was no case in which a positive margin was detected only in the simulated conventional assessment. Conclusions The whole-mount technique is more sensitive than conventional assessment for identifying a positive margin or multifocal disease in breast lumpectomy specimens. Undersampling in conventional sections was implicated in almost all cases of discordance. The majority of positive margins or secondary foci identified only in whole-mount serial sections concerned in-situ disease. [ABSTRACT FROM AUTHOR]

Published

2016

6. A novel, automated technology for multiplex biomarker imaging and application to breast cancer.

Author

Clarke, Gina M, Zubovits, Judit T, Shaikh, Kashan A, Wang, Dan, Dinn, Sean R, Corwin, Alex D, Santamaria‐Pang, Alberto, Li, Qing, Nofech‐Mozes, Sharon, Liu, Kela, Pang, Zhengyu, Filkins, Robert J, and Yaffe, Martin J

Subjects

*BIOMARKERS, *BREAST cancer, *PROTEINS, *IMMUNOFLUORESCENCE, *HORMONE receptors

Abstract

Aims Multiplexed immunofluorescence is a powerful tool for validating multigene assays and understanding the complex interplay of proteins implicated in breast cancer within a morphological context. We describe a novel technology for imaging an extended panel of biomarkers on a single, formalin-fixed paraffin-embedded breast sample and evaluating biomarker interaction at a single-cell level, and demonstrate proof-of-concept on a small set of breast tumours, including those which co-express hormone receptors with Her2/neu and Ki-67. Methods and results Using a microfluidic flow cell, reagent exchange was automated and consisted of serial rounds of staining with dye-conjugated antibodies, imaging and chemical deactivation. A two-step antigen retrieval process was developed to satisfy all epitopes simultaneously, and key parameters were optimized. The imaging sequence was applied to seven breast tumours, and compared with conventional immunohistochemistry. Single-cell correlation analysis was performed with automated image processing. Conclusions We have described a novel platform for evaluating biomarker co-localization. Expression in multiplexed images is consistent with conventional immunohistochemistry. Automation reduces inconsistencies in staining and positional shifts, while the fluorescent dye cycling approach dramatically expands the number of biomarkers which can be visualized and quantified on a single tissue section. [ABSTRACT FROM AUTHOR]

Published

2014

7. Development and evaluation of a robust algorithm for computer-assisted detection of sentinel lymph node micrometastases.

Author

Clarke, Gina M., Peressotti, Chris, Holloway, Claire M. B., Zubovits, Judit T., Liu, Kela, and Yaffe, Martin J.

Subjects

*MICROSCOPY, *IMMUNOHISTOCHEMISTRY, *COMPUTER assisted instruction, *METASTASIS, *CANCER cells, *DIAGNOSIS, CANCER diagnostic equipment

Abstract

Aims: Increasing the sectioning rate for breast sentinel lymph nodes can increase the likelihood of detecting micrometastases. To make serial sectioning feasible, we have developed an algorithm for computer-assisted detection (CAD) with digitized lymph node sections. Methods and results: K-means clustering assigned image pixels to one of four areas in a colourspace (representing tumour, unstained background, counterstained background and microtomy artefacts). Four filters then removed 'false-positive' pixels from the tumour cluster. A set of 43 sections containing tumour (a total of 259 foci) and 59 sections negative for malignancy was defined by two pathologists, using light microscopy, and CAD was applied. For the clinically relevant task of identifying the largest focus in each section (micrometastasis in 22 / 43 sections), the sensitivity and specificity were 100%. Isolated tumour cells (ITCs) were identified in one slide initially considered to be negative. Identification of all 259 foci yielded sensitivities of 57.5% for ITCs (<0.200 mm), 89.5% for micrometastases, and 100% for larger metastases, with one false-positive. Reduced sensitivity was ascribed to variable staining. Nine additional metastases (<0.01-0.3 mm) that were not initially identified were detected by CAD. Conclusions: This algorithm is well suited to the task of sentinel lymph node evaluation and may enhance the detection of occult micrometastases. [ABSTRACT FROM AUTHOR]

Published

2011