Your search keyword '"Teh M"' showing total 81 results

1. 4CPS-110 Systematic review and e-questionnaire on the service characteristics, operations and activities of centres for medicines information (CMI)

Author

van den broucke, E, primary, Cosemans, L, additional, Min Teh, M, additional, de Rijdt, T, additional, Quintens, C, additional, and Spriet, I, additional

Published

2024

2. Australia’s Identified Mineral Resources 2021

Author

Senior, A., primary, Britt, A, additional, Pheeney, J, additional, Summerfield, D, additional, Hughes, A, additional, Hitchman, A, additional, Cross, A, additional, Sexton, M, additional, and Teh, M, additional

Published

2022

3. Australia's indentified mineral resources 2020

Author

Senior, A., primary, Britt, A., additional, Summerfield, D., additional, Hughes, A., additional, Hitchman, A., additional, Cross, A., additional, Champion, D., additional, Huston, D., additional, Bastrakov, E., additional, Sexton, M., additional, Maloney, J., additional, Pheeney, J., additional, Teh, M., additional, and Schofield, A., additional

Published

2021

4. Minerals on the edge: sediment-hosted base metal endowment above steps in lithospheric thickness

Author

Czarnota, K., primary, Hoggard, M.J., additional, Richards, F.D., additional, Teh, M., additional, Huston, D.L., additional, Jaques, A.L., additional, and Ghelichkhan, S., additional

Published

2020

5. The interferon stimulated gene viperin, restricts Shigella. flexneri in vitro

Author

Helbig, K. J., Teh, M. Y., Crosse, K. M., Monson, E. A., Smith, M., Tran, E. N., Standish, A. J., Morona, R., and Beard, M. R.

Published

2019

6. PL02.14 Triaging ILST Screening Participants at Program Entry: Comparative Performance of PanCan versus LungRADSv1.1 Protocol.

Author

McWilliams, A.M., Tammemagi, M., Atkar-Khattra, S., Mayo, J., Meyers, R., Yee, J., English, J., Marshall, H., Passmore, L., Bowman, R., Yang, I., Brims, F., Logan, J., Lim, K.P., Mo, L., Melsom, S., Saffar, B., Kwok, Y., Sheehan, R., and Teh, M.

Published

2024

7. USPSTF2013 versus PLCOm2012 lung cancer screening eligibility criteria (International Lung Screening Trial): interim analysis of a prospective cohort study

Author

Tammemagi, MC, Ruparel, M, Tremblay, A, Myers, R, Mayo, J, Yee, J, Atkar-Khattra, S, Yuan, R, Cressman, S, English, J, Bedard, E, MacEachern, P, Burrowes, P, Quaife, SL, Marshall, H, Yang, I, Bowman, R, Passmore, L, McWilliams, A, Brims, F, Lim, KP, Mo, L, Melsom, S, Saffar, B, Teh, M, Sheehan, R, Kuok, Y, Manser, R, Irving, L, Steinfort, D, McCusker, M, Pascoe, D, Fogarty, P, Stone, E, Lam, DCL, Ng, M-Y, Vardhanabhuti, V, Berg, CD, Hung, RJ, Janes, SM, Fong, K, Lam, S, Tammemagi, MC, Ruparel, M, Tremblay, A, Myers, R, Mayo, J, Yee, J, Atkar-Khattra, S, Yuan, R, Cressman, S, English, J, Bedard, E, MacEachern, P, Burrowes, P, Quaife, SL, Marshall, H, Yang, I, Bowman, R, Passmore, L, McWilliams, A, Brims, F, Lim, KP, Mo, L, Melsom, S, Saffar, B, Teh, M, Sheehan, R, Kuok, Y, Manser, R, Irving, L, Steinfort, D, McCusker, M, Pascoe, D, Fogarty, P, Stone, E, Lam, DCL, Ng, M-Y, Vardhanabhuti, V, Berg, CD, Hung, RJ, Janes, SM, Fong, K, and Lam, S

Abstract

BACKGROUND: Lung cancer is a major health problem. CT lung screening can reduce lung cancer mortality through early diagnosis by at least 20%. Screening high-risk individuals is most effective. Retrospective analyses suggest that identifying individuals for screening by accurate prediction models is more efficient than using categorical age-smoking criteria, such as the US Preventive Services Task Force (USPSTF) criteria. This study prospectively compared the effectiveness of the USPSTF2013 and PLCOm2012 model eligibility criteria. METHODS: In this prospective cohort study, participants from the International Lung Screening Trial (ILST), aged 55-80 years, who were current or former smokers (ie, had ≥30 pack-years smoking history or ≤15 quit-years since last permanently quitting), and who met USPSTF2013 criteria or a PLCOm2012 risk threshold of at least 1·51% within 6 years of screening, were recruited from nine screening sites in Canada, Australia, Hong Kong, and the UK. After enrolment, patients were assessed with the USPSTF2013 criteria and the PLCOm2012 risk model with a threshold of at least 1·70% at 6 years. Data were collected locally and centralised. Main outcomes were the comparison of lung cancer detection rates and cumulative life expectancies in patients with lung cancer between USPSTF2013 criteria and the PLCOm2012 model. In this Article, we present data from an interim analysis. To estimate the incidence of lung cancers in individuals who were USPSTF2013-negative and had PLCOm2012 of less than 1·51% at 6 years, ever-smokers in the Prostate Lung Colorectal and Ovarian Cancer Screening Trial (PLCO) who met these criteria and their lung cancer incidence were applied to the ILST sample size for the mean follow-up occurring in the ILST. This trial is registered at ClinicalTrials.gov, NCT02871856. Study enrolment is almost complete. FINDINGS: Between June 17, 2015, and Dec 29, 2020, 5819 participants from the International Lung Screening Trial (ILST) were enr

Published

2022

8. An Immunohistochemical and Histological Study of the Animal Periodontal Ligament During Orthodontic Force Application with Concomitant Application of Electric Current - An Animal Study

Author

Teh Min Chou, Ashish Agarwal, and Rahul Agarwal

Subjects

electrical stimulation, pdl remodelling, rate of tooth movement, Dentistry, RK1-715

Abstract

Introduction: The application of direct current can have a significant impact on the rate of tooth movement and surrounding periodontal ligament collagen turnover. This study aims to provide insight into the optimal characteristics of applied current to achieve enhanced tissue response. Method: Eighteen male Wistar rats were divided into three groups (I, II, and III). Split mouth design was used, and each side was allocated into an experimental group or control group. Experimental sides of groups I, II, and III received 20, 10, and 15 μA of current (15 min, twice daily for 3 days). Both the experimental and control groups receive an orthodontic force via the NiTi closed coil spring. The amount of tooth movement was determined daily. Immunohistochemistry slides were scored using the immunoreactive scoring (IRS) system for collagen types I and III. One-way Analysis of Variance (ANOVA) and Tukey post hoc test were used to analyse the rate of tooth movement, while Mann–Whitney test was used to analyse IRS distribution between control and experimental groups. Results: Compared with the control group, there was a statistically significant difference in tooth movement in all the experimental groups, with group 3 showing the maximum rate on days 2 and 3. This was supported by immunoreactive scores for both collagen types I and III. Conclusions: After 72 hours, the expression of collagen types 1 and 3 increased significantly for group III. This finding was in harmony with the rate of tooth movement, which was maximum for group 3 (15 μA) as compared to other groups.

Published

2024

9. # 1570 Identification of individuals at high risk of gastric cancer for targeted endoscopic screening

Author

ZHU, F, LIM, L L, KOH, C KY, LEE, S E, ONG, DEH, LIM, L G, HO, K Y, CHIA, C K, KHOR, C JL, OOI, C J, FOCK, K M, SO, J BY, LIM, W C, LING, K L, ANG, T L, WONG, A S, RAO, J, RAJNAKOVA, A, TEH, M, SALTO-TELLEZ, M, SRIVASTAVA, S, TEO, Y Y, and YEOH, K G

Published

2015

10. R36 Computational Flow Dynamics in Ascending Aortic Aneurysm – A CT Survey

Author

Jenkinson, C., primary, Wood, T., additional, Teh, M., additional, and Joshi, P., additional

Published

2021

11. Rethinking Urban Public Space: Physical and Functional Analysis through Visual Surveys

Author

Abdul Rahman, N, primary, Ghani, I, additional, Teh, M Z, additional, and Ibrahim, K A, additional

Published

2020

12. A loss-of-function mutation inItgalcontributes to the high susceptibility of Collaborative Cross strain CC042 toSalmonellainfections

Author

Jing Zhang, Jamie Kim, Teh M, Danielle Malo, Anastasia Nijnik, Meade R, Romain Cayrol, Xavier Montagutelli, Jean Jaubert, and Megan M. Eva

Subjects

Salmonella, education.field_of_study, Intracellular parasite, Integrin Alpha-L, Population, Salmonella infection, Biology, medicine.disease, medicine.disease_cause, Microbiology, Immune system, medicine, education, Gene, CD8

Abstract

Salmonellaare intracellular bacteria that are found in the gastrointestinal tract of mammalian, avian, and reptilian hosts. They are one of the leading causes of foodborne infections and a major threat for human populations worldwide. Mouse models have been extensively used to model distinct aspects of the humanSalmonellainfectionsin vivoand have led to the identification of several host susceptibility genes. We have investigated the susceptibility of Collaborative Cross strains to intravenous infection withSalmonellaTyphimurium as a model of human systemic invasive infection. In this model, strain CC042 displayed extreme susceptibility with very high bacterial loads and mortality. CC042 mice showed lower spleen weight and decreased splenocyte numbers before and after infection, affecting mostly CD8+T cells, B cells, and all myeloid populations. Uninfected mice also had lower thymus weight with reduced total number of thymocytes and double negative and (CD4+, CD8+) double positive thymocytes. Analysis of bone marrow resident hematopoietic progenitors showed a strong bias against lymphoid primed multipotent progenitors, which are the precursors of T, B and NK cells. An F2 cross between CC042 and C57BL/6N identified two significant QTLs on chromosome 7 (Stsl6andStsl7) with WSB-derived susceptible alleles. A private variant in the integrin alpha L (Itgal) gene is carried by CC042 in theStsl7QTL region. A quantitative complementation test confirmed the impact ofItgalloss of function in a (C57BL/6JxCC042)F1 background, but not in a C57BL/6J inbred background. These results further emphasize the utility of the Collaborative Cross to identify new host genetic variants controlling susceptibility to infections and improve our understanding of the function of theItgalgene.Author summarySalmonellaare one of the leading causes of foodborne infections and a major threat for human populations worldwide. Not all humans are equally susceptible toSalmonellainfection. Some individuals will develop minor symptoms and recover while others develop severe illness and might die. Mouse models are used to study distinct aspects of humanSalmonellainfectionin vivo. We used a new genetically diverse mouse population to investigate host susceptibility differences toSalmonellainfection. We identified one mouse strain with an extreme susceptibility to infection characterized by very high bacterial loads and mortality. Mice of this strain had small thymus and spleen, two organs which are very important for producing a fully mature immune system. We showed that the strain’s immune response is impaired and that its extreme susceptibility toSalmonellainfection is due to multiple genes defects. We identified a loss-of-function mutation in theItgalgene (Integrin Subunit Alpha L) that plays a central role in the immune response to infection. This gene explains part of the susceptibility and other gene(s) involved remain to be identified. Our results emphasize how new genetically diverse animal models can lead to the identification of new host genetic variants controlling susceptibility to pathogens and improve our understanding of human infections.

Published

2019

13. Impact of COVID-19 on Breast Cancer Management in a Multiethnic Middle-Income Asian Country Setting

Author

Ng Jing Hui, See Mee Hoong, Tneoh Jia Min, Teh Mei Sze, Mahmoud Danaee, Nur Shahirah Abdul Latiff, Abigail Ashwini Murali, and Lee Lee Lai

Subjects

breast neoplasm, pandemic, therapeutic, patient, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Medicine

Abstract

Objective:Coronavirus disease-2019 (COVID-19) has caused hospitals to suspend routine procedures. As the world recovers, there is concern that the outcome of many diseases has been impaired. This study aimed to assess the impact of the pandemic on breast cancer demography, clinicopathological characteristics and patient management at a teaching hospital in Kuala Lumpur, Malaysia.Materials and Methods:Pre-COVID data were collected between January 1, 2019, to March 18, 2020, when a national lockdown was implemented, which caused the suspension of services at the breast clinic of University Malaya Medical Centre (UMMC). COVID data was obtained from March 2020 until June 2021.Results:This study compared 374 breast cancer patients in the COVID-19 period with 382 patients in the pre-COVID period. There was no significant difference in the median (range) time to surgery between pre-COVID [45 (26.50–153.50) days] and COVID [44 (24.75–156.25) days] periods. The clinicopathological features of breast cancer showed reduction in in situ carcinoma and increase in Stage 4 diagnoses during the COVID period. There was a reduction in screening-detected carcinoma (9% vs. 12.3%), mastectomy followed by immediate reconstruction (5.6% vs. 14.5%) and adjuvant chemotherapy (25.8% vs. 32.9%) in the COVID period.Conclusion:In this center COVID-19 caused operational changes in breast cancer management, including a reduction in reconstructive procedures and adjuvant treatment. Healthcare disruption and fear of COVID may have caused delayed diagnosis, resulting in a higher frequency of Stage 4 disease and lower proportion of in situ carcinoma during the pandemic. However, there was no delay in the time to surgery, reduction in surgical volume, or change in surgery types.

Published

2023

14. The Pemphigus Vulgaris antigen desmoglein-3 suppresses p53 function via the YAP-Hippo pathway

Author

Rehman, Ambreen, primary, Cai, Yang, additional, Hünefeld, Christian, additional, Jedličková, Hana, additional, Huang, Yunying, additional, Teh, M Teck, additional, Uttagomol, Jutamas, additional, Kang, Angray, additional, Warnes, Gary, additional, Ahmad, Usama, additional, Harwood, Catherine, additional, Bergamaschi, Daniele, additional, Parkinson, Eric Kenneth, additional, Röcken, Martin, additional, Hart, Ian, additional, and Wan, Hong, additional

Published

2018

15. SYSTEMATIC REVIEW AND E-QUESTIONNAIRE ON THE SERVICE CHARACTERISTICS, OPERATIONS AND ACTIVITIES OF CENTRES FOR MEDICINES INFORMATION (CMI).

Author

van den broucke, E., Cosemans, L., Min Teh, M., de Rijdt, T., Quintens, C., and Spriet, I.

Published

2024

16. Eosinophilic oesophagitis in children: an uncommon occurrence in a predominantly Chinese population in Singapore

Author

Tan, LN, primary, Srivastava, S, additional, Teh, M, additional, Quak, SH, additional, and Aw, MM, additional

Published

2017

17. Manganese(I)-Catalyzed C-H Activation:The Key Role of a 7-Membered Manganacycle in H-Transfer and Reductive Elimination

Author

Yahaya, NP, Appleby, KM, Teh, M, Wagner, C, Troschke, E, Bray, JT, Duckett, SB, Hammarback, LA, Ward, JS, Milani, J, Pridmore, NE, Whitwood, AC, Lynam, JM, Fairlamb, IJ, Yahaya, NP, Appleby, KM, Teh, M, Wagner, C, Troschke, E, Bray, JT, Duckett, SB, Hammarback, LA, Ward, JS, Milani, J, Pridmore, NE, Whitwood, AC, Lynam, JM, and Fairlamb, IJ

Abstract

Manganese-catalyzed C−H bond activation chemistry is emerging as a powerful and complementary method for molecular functionalization. A highly reactive seven-membered MnI intermediate is detected and characterized that is effective for H-transfer or reductive elimination to deliver alkenylated or pyridinium products, respectively. The two pathways are determined at MnI by judicious choice of an electron-deficient 2-pyrone substrate containing a 2-pyridyl directing group, which undergoes regioselective C−H bond activation, serving as a valuable system for probing the mechanistic features of Mn C−H bond activation chemistry.

Published

2016

18. Sa2035 Fiber-Optic Raman Spectroscopy for Label-Free In Vivo Molecular Diagnostics of Gastrointestinal Neoplasia at Endoscopy

Author

Zheng, Wei, primary, Lin, Kan, additional, Wang, J, additional, Ho, KY, additional, Teh, M, additional, Yeoh, KG, additional, So, Jimmy B., additional, Shabbir, A, additional, and Huang, Zhiwei, additional

Published

2016

19. Description and preliminary results from a structured specialist behavioural weight management group intervention: Specialist Lifestyle Management (SLiM) programme

Author

Brown, A., primary, Gouldstone, A., additional, Fox, E., additional, Field, A., additional, Todd, W., additional, Shakher, J., additional, Bellary, S., additional, Teh, M. M., additional, Azam, M., additional, John, R., additional, Jagielski, A., additional, Arora, T., additional, Thomas, G. N., additional, and Taheri, S., additional

Published

2015

20. PHYLOGENETIC RELATIONSHIPS OF THE ORANG ASLI (PROTO MALAY) TRIBE BASED ON THE HVS II GENE SEQUENCES.

Author

MD-ZAIN, B. M., TEH, M. S., ANG, K. C., LIM, L. S., and YAAKOP, S.

Subjects

*ORANG Asal (Malaysian people), *PHYLOGENY

Abstract

The Proto Malays are the second largest Orang Asli tribe in Peninsular Malaysia. There are six subtribes of Proto Malays, namely the Jakun, Kanaq, Kuala/Laut, Seletar, Temuan and Semelai. Very little is known about the phylogenetic relationships among the Proto Malay subtribes. This study aims to reveal the phylogenetic relationships of the Proto Malays using HVS II D-Loop sequences. Blood samples were collected from all six subtribes. DNA was extracted and 369 bp of HVS II (D-Loop region) was amplified. Phylogenetic trees were constructed using Maximum Parsimony (MP) and the Neighbour Joining (NJ) method. The HVS II D-Loop gene sequence analysis revealed close phylogenetic relationships between all the Proto Malay subtribes as they can be assembled into a single clade. Amongst all the Proto Malay subtribes, the Kanaq shared the closest phylogenetic relationships among themselves with the lowest pairwise genetic distance of 0.0055 and they also formed a monophyletic clade in the NJ and MP tree. The NJ tree explained the phylogenetic relationships of the Proto Malay subtribes the best, as it portrayed the genetic distances of the subjects involved apart from the branching patterns. This study provides an insight into how different Proto Malay subtribes are genetically related to each other although their physical attributes may differ. It also distinguishes the uniqueness of each subtribe based on their genetics. [ABSTRACT FROM AUTHOR]

Published

2017

21. IQGAP3 signalling mediates intratumoral functional heterogeneity to enhance malignant growth.

Author

Shimura M, Matsuo J, Pang S, Jangphattananont N, Hussain A, Rahmat MB, Lee JW, Douchi D, Tong JJL, Myint K, Srivastava S, Teh M, Koh V, Yong WP, So JBY, Tan P, Yeoh KG, Unno M, Chuang LSH, and Ito Y

Abstract

Background: The elevation of IQGAP3 expression in diverse cancers indicates a key role for IQGAP3 in carcinogenesis. Although IQGAP3 was established as a proliferating stomach stem cell factor and a regulator of the RAS-ERK pathway, how it drives cancer growth remains unclear., Objective: We define the function of IQGAP3 in gastric cancer (GC) development and progression., Design: We studied the phenotypic changes caused by IQGAP3 knockdown in three molecularly diverse GC cell lines by RNA-sequencing. In vivo tumorigenesis and lung metastasis assays corroborated IQGAP3 as a mediator of oncogenic signalling. Spatial analysis was performed to evaluate the intratumoral transcriptional and functional differences between control tumours and IQGAP3 knockdown tumours., Results: Transcriptomic profiling showed that IQGAP3 inhibition attenuates signal transduction networks, such as KRAS signalling, via phosphorylation blockade. IQGAP3 knockdown was associated with significant inhibition of MEK/ERK signalling-associated growth factors, including TGFβ1, concomitant with gene signatures predictive of impaired tumour microenvironment formation and reduced metastatic potential. Xenografts involving IQGAP3 knockdown cells showed attenuated tumorigenesis and lung metastasis in immunodeficient mice. Accordingly, immunofluorescence staining revealed significant reductions of TGFβ/SMAD signalling and αSMA-positive stromal cells; digital spatial analysis indicated that IQGAP3 is indispensable for the formation of two phenotypically diverse cell subpopulations, which played crucial but distinct roles in promoting oncogenic functions., Conclusion: IQGAP3 knockdown suppressed the RAS-TGFβ signalling crosstalk, leading to a significant reduction of the tumour microenvironment. In particular, IQGAP3 maintains functional heterogeneity of cancer cells to enhance malignant growth. IQGAP3 is thus a highly relevant therapy target in GC., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2024

22. CEACAM5 and TROP2 define metaplastic and dysplastic transitions in human antral gastric precancerous lesions and tumors.

Author

Jang B, Lee SH, Dovirak I, Kim H, Srivastava S, Teh M, Yeoh KG, So JB, Tsao SKK, Khor CJ, Ang TL, and Goldenring JR

Subjects

Humans, Gastric Mucosa pathology, Metaplasia, Carcinoembryonic Antigen, GPI-Linked Proteins metabolism, Stomach Neoplasms pathology, Precancerous Conditions pathology

Abstract

Background: Mucosal gastric atrophy and intestinal metaplasia (IM) increase the risk for the development of gastric cancer (GC) as they represent a field for development of dysplasia and intestinal-type gastric adenocarcinoma., Methods: We have investigated the expression of two dysplasia markers, CEACAM5 and TROP2, in human antral IM and gastric tumors to assess their potential as molecular markers., Results: In the normal antral mucosa, weak CEACAM5 and TROP2 expression was only observed in the foveolar epithelium, while inflamed antrum exhibited increased expression of both markers. Complete IM exhibited weak CEACAM5 expression at the apical surface, but no basolateral TROP2 expression. On the other hand, incomplete IM demonstrated high levels of both CEACAM5 and TROP2 expression. Notably, incomplete IM with dysplastic morphology (dysplastic incomplete IM) exhibited higher levels of CEACAM5 and TROP2 expression compared to incomplete IM without dysplastic features (simple incomplete IM). In addition, dysplastic incomplete IM showed diminished SOX2 and elevated CDX2 expression compared to simple incomplete IM. CEACAM5 and TROP2 positivity in incomplete IM was similar to that of gastric adenomas and GC. Significant association was found between CEACAM5 and TROP2 positivity and histology of GC., Conclusions: These findings support the concept that incomplete IM is more likely associated with GC development. Overall, our study provides evidence of the heterogeneity of gastric IM and the distinct expression profiles of CEACAM5 and TROP2 in dysplastic incomplete IM. Our findings support the potential use of CEACAM5 and TROP2 as molecular markers for identifying individuals with a higher risk of GC development in the context of incomplete IM., (© 2024. The Author(s) under exclusive licence to The International Gastric Cancer Association and The Japanese Gastric Cancer Association.)

Published

2024

23. Spatiotemporal genomic profiling of intestinal metaplasia reveals clonal dynamics of gastric cancer progression.

Author

Huang KK, Ma H, Chong RHH, Uchihara T, Lian BSX, Zhu F, Sheng T, Srivastava S, Tay ST, Sundar R, Tan ALK, Ong X, Lee M, Ho SWT, Lesluyes T, Ashktorab H, Smoot D, Van Loo P, Chua JS, Ramnarayanan K, Lau LHS, Gotoda T, Kim HS, Ang TL, Khor C, Lee JWJ, Tsao SKK, Yang WL, Teh M, Chung H, So JBY, Yeoh KG, and Tan P

Subjects

Humans, Prospective Studies, Gastric Mucosa pathology, Genomics, Metaplasia genetics, Stomach Neoplasms genetics, Stomach Neoplasms metabolism, Precancerous Conditions genetics

Abstract

Intestinal metaplasia (IM) is a pre-malignant condition of the gastric mucosa associated with increased gastric cancer (GC) risk. Analyzing 1,256 gastric samples (1,152 IMs) across 692 subjects from a prospective 10-year study, we identify 26 IM driver genes in diverse pathways including chromatin regulation (ARID1A) and intestinal homeostasis (SOX9). Single-cell and spatial profiles highlight changes in tissue ecology and IM lineage heterogeneity, including an intestinal stem-cell dominant cellular compartment linked to early malignancy. Expanded transcriptome profiling reveals expression-based molecular subtypes of IM associated with incomplete histology, antral/intestinal cell types, ARID1A mutations, inflammation, and microbial communities normally associated with the healthy oral tract. We demonstrate that combined clinical-genomic models outperform clinical-only models in predicting IMs likely to transform to GC. By highlighting strategies for accurately identifying IM patients at high GC risk and a role for microbial dysbiosis in IM progression, our results raise opportunities for GC precision prevention and interception., Competing Interests: Declaration of interests P.T. has stock in Tempus Healthcare, previous funding from Kyowa Hakko Kirin and Thermo Fisher Scientific, and patents/other intellectual property through the Agency for Science and Technology Research, Singapore (all outside the submitted work). K.G.Y. is a co-inventor on patents “Serum MicroRNA Biomarker for the Diagnosis of Gastric Cancer” and “Methods Related to Real-Time Cancer Diagnostics at Endoscopy Utilizing Fiber-Optic Raman Spectroscopy”; a member of Scientific Advisory Board of MiRXES Pte Ltd. He has no stock or shares in the related companies. He has no conflicts of interest to disclose regarding this submitted work. R.S. has received honoraria from MSD, Eli Lilly, BMS, Roche, Taiho, Astra Zeneca, DKSH, and Ipsen; has advisory activity with Bristol Myers Squibb, Merck, Eisai, Bayer, Taiho, Novartis, MSD, GSK, DKSH, and Astellas; received research funding from Paxman Coolers, MSD, and Natera; and has received travel grants from Roche, Astra Zeneca, Taiho, Eisai, and DKSH., (Copyright © 2023 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2023

24. Predictors of SARS-CoV-2 Omicron breakthrough infection after receipt of AZD7442 (tixagevimab-cilgavimab) for pre-exposure prophylaxis among hematologic malignancy patients.

Author

Laracy JC, Yan J, Steiger SN, Tan CA, Cohen N, Robilotti EV, Fender J, Cohen S, Korde N, Lee-Teh M, Noy A, Oved JH, Roeker LE, Shah G, Babady NE, Kamboj M, and Seo SK

Subjects

Humans, SARS-CoV-2, Breakthrough Infections, Retrospective Studies, Antibodies, Monoclonal, COVID-19 prevention & control, Pre-Exposure Prophylaxis, Hematologic Neoplasms complications, Hematologic Neoplasms drug therapy

Abstract

AZD7442 (tixagevimab-cilgavimab) is a combination of two human monoclonal antibodies for pre-exposure prophylaxis of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection among high-risk patients who do not mount a reliable vaccine response. Foremost among these are hematologic malignancy patients with limited clinical trial or realworld experience to assess the effectiveness of this combination treatment since the emergence of Omicron and its subvariants. We performed a retrospective study of 892 high-risk hematologic malignancy patients who received AZD7442 at Memorial Sloan Kettering Cancer Center in New York City from January 1, 2022 to July 31, 2022. We evaluated demographic, clinical, and laboratory characteristics and performed regression analyses to evaluate risk factors for breakthrough infection. We also evaluated the impact of updated AZD7442 dosing regimens on the risk of breakthrough infection. Among 892 patients, 98 (10.9%) had a breakthrough infection during the study period. A majority received early outpatient treatment (82%) and eventually eight (8.2%) required hospitalization for management of Coronavirus Disease 2019 (COVID-19), with a single instance of severe COVID-19 and death. Patients who received a repeat dose or a higher firsttime dose of AZD7442 had a lower incidence of breakthrough infection. Univariate analyses did not reveal any significant predictors of breakthrough infection. While AZD7442 is effective at reducing SARS-CoV-2 breakthrough infection in patients with hematologic malignancies, no risk factors reliably predicted risk of infection. Patients who received updated dosing regimens as per Food and Drug Administration guidelines had better protection against breakthrough infection.

Published

2023

25. Ancient genomic linkage couples metabolism with erythroid development.

Author

Preston AE, Frost JN, Badat M, Teh M, Armitage AE, Norfo R, Wideman SK, Hanifi M, White N, Roy N, Ghesquiere B, Babbs C, Kassouf M, Davies J, Hughes JR, Beagrie R, Higgs DR, and Drakesmith H

Abstract

Generation of mature cells from progenitors requires tight coupling of differentiation and metabolism. During erythropoiesis, erythroblasts are required to massively upregulate globin synthesis then clear extraneous material and enucleate to produce erythrocytes 1-3 . Nprl3 has remained in synteny with the α-globin genes for >500 million years 4 , and harbours the majority of the α-globin enhancers 5 . Nprl3 is a highly conserved inhibitor of mTORC1, which controls cellular metabolism. However, whether Nprl3 itself serves an erythroid role is unknown. Here, we show that Nprl3 is a key regulator of erythroid metabolism. Using Nprl3-deficient fetal liver and adult competitive bone marrow - fetal liver chimeras, we show that NprI3 is required for sufficient erythropoiesis. Loss of Nprl3 elevates mTORC1 signalling, suppresses autophagy and disrupts erythroblast glycolysis and redox control. Human CD34+ progenitors lacking NPRL3 produce fewer enucleated cells and demonstrate dysregulated mTORC1 signalling in response to nutrient availability and erythropoietin. Finally, we show that the α-globin enhancers upregulate NprI3 expression, and that this activity is necessary for optimal erythropoiesis. Therefore, the anciently conserved linkage of NprI3 , α-globin and their associated enhancers has enabled coupling of metabolic and developmental control in erythroid cells. This may enable erythropoiesis to adapt to fluctuating nutritional and environmental conditions.

Published

2023

26. RUNX3 inactivates oncogenic MYC through disruption of MYC/MAX complex and subsequent recruitment of GSK3β-FBXW7 cascade.

Author

Oei V, Chuang LSH, Matsuo J, Srivastava S, Teh M, and Ito Y

Subjects

Animals, Mice, Cell Line, Tumor, F-Box-WD Repeat-Containing Protein 7 metabolism, Glycogen Synthase Kinase 3 beta genetics, Glycogen Synthase Kinase 3 beta metabolism, Proteolysis, Cell Nucleus metabolism, Lung Neoplasms genetics, Lung Neoplasms metabolism, Core Binding Factor Alpha 3 Subunit genetics, Core Binding Factor Alpha 3 Subunit metabolism

Abstract

MYC is one of the most commonly dysregulated proto-oncogenes in cancer. MYC promotes cancer initiation and maintenance by regulating multiple biological processes, such as proliferation and stem cell function. Here, we show that developmental regulator RUNX3 targets MYC protein for rapid degradation through the glycogen synthase kinase-3 beta-F-box/WD repeat-containing protein 7 (GSK3β-FBXW7) proteolytic pathway. The evolutionarily conserved Runt domain of RUNX3 interacts directly with the basic helix-loop-helix leucine zipper of MYC, resulting in the disruption of MYC/MAX and MYC/MIZ-1 interactions, enhanced GSK3β-mediated phosphorylation of MYC protein at threonine-58 and its subsequent degradation via the ubiquitin-proteasomal pathway. We therefore uncover a previously unknown mode of MYC destabilization by RUNX3 and provide an explanation as to why RUNX3 inhibits early-stage cancer development in gastrointestinal and lung mouse cancer models., (© 2023. The Author(s).)

Published

2023

27. Regulatory enhancer profiling of mesenchymal-type gastric cancer reveals subtype-specific epigenomic landscapes and targetable vulnerabilities.

Author

Ho SWT, Sheng T, Xing M, Ooi WF, Xu C, Sundar R, Huang KK, Li Z, Kumar V, Ramnarayanan K, Zhu F, Srivastava S, Isa ZFBA, Anene-Nzelu CG, Razavi-Mohseni M, Shigaki D, Ma H, Tan ALK, Ong X, Lee MH, Tay ST, Guo YA, Huang W, Li S, Beer MA, Foo RSY, Teh M, Skanderup AJ, Teh BT, and Tan P

Subjects

Humans, Cisplatin metabolism, Cisplatin therapeutic use, Prospective Studies, Protein Kinases genetics, Repressor Proteins, Retrospective Studies, Gene Expression Regulation, Neoplastic, Stomach Neoplasms genetics, Epigenesis, Genetic, Enhancer Elements, Genetic

Abstract

Objective: Gastric cancer (GC) comprises multiple molecular subtypes. Recent studies have highlighted mesenchymal-subtype GC (Mes-GC) as a clinically aggressive subtype with few treatment options. Combining multiple studies, we derived and applied a consensus Mes-GC classifier to define the Mes-GC enhancer landscape revealing disease vulnerabilities., Design: Transcriptomic profiles of ~1000 primary GCs and cell lines were analysed to derive a consensus Mes-GC classifier. Clinical and genomic associations were performed across >1200 patients with GC. Genome-wide epigenomic profiles (H3K27ac, H3K4me1 and assay for transposase-accessible chromatin with sequencing (ATAC-seq)) of 49 primary GCs and GC cell lines were generated to identify Mes-GC-specific enhancer landscapes. Upstream regulators and downstream targets of Mes-GC enhancers were interrogated using chromatin immunoprecipitation followed by sequencing (ChIP-seq), RNA sequencing, CRISPR/Cas9 editing, functional assays and pharmacological inhibition., Results: We identified and validated a 993-gene cancer-cell intrinsic Mes-GC classifier applicable to retrospective cohorts or prospective single samples. Multicohort analysis of Mes-GCs confirmed associations with poor patient survival, therapy resistance and few targetable genomic alterations. Analysis of enhancer profiles revealed a distinctive Mes-GC epigenomic landscape, with TEAD1 as a master regulator of Mes-GC enhancers and Mes-GCs exhibiting preferential sensitivity to TEAD1 pharmacological inhibition. Analysis of Mes-GC super-enhancers also highlighted NUAK1 kinase as a downstream target, with synergistic effects observed between NUAK1 inhibition and cisplatin treatment., Conclusion: Our results establish a consensus Mes-GC classifier applicable to multiple transcriptomic scenarios. Mes-GCs exhibit a distinct epigenomic landscape, and TEAD1 inhibition and combinatorial NUAK1 inhibition/cisplatin may represent potential targetable options., Competing Interests: Competing interests: PT has stock and other ownership interests in Tempus Healthcare, previous research funding from Kyowa Hakko Kirin and Thermo Fisher Scientific, and patents/other intellectual property through the Agency for Science and Technology Research, Singapore (all outside the submitted work). RS has received honoraria from MSD, Eli Lilly, Bristol Myers Squibb, Roche, Taiho, Astra Zeneca and DKSH; has advisory activity with Bristol Myers Squibb, Merck, Eisai, Bayer, Taiho, Novartis, MSD and GSK; received research funding from MSD and Paxman Coolers; and has received travel grants from Astra Zeneca, Eisai, Roche, Taiho and DKSH. All remaining authors have declared no conflicts of interest., (© Author(s) (or their employer(s)) 2023. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2023

28. Academy of Medicine, Singapore clinical guideline on endoscopic surveillance and management of gastric premalignant lesions.

Author

Namasivayam V, Koh CJ, Tsao S, Lee J, Ling KL, Khor C, Lim T, Li JW, Oo AM, Yip BCH, Hussain I, Chua TS, Toh BC, Ong HS, Wang LM, So JBY, Teh M, Yeoh KG, and Ang TL

Subjects

Adenomatous Polyps, Endoscopy, Humans, Singapore, Precancerous Conditions diagnosis, Precancerous Conditions epidemiology, Precancerous Conditions therapy, Stomach Neoplasms diagnosis, Stomach Neoplasms therapy

Abstract

Gastric cancer (GC) has a good prognosis, if detected at an early stage. The intestinal subtype of GC follows a stepwise progression to carcinoma, which is treatable with early detection and intervention using high-quality endoscopy. Premalignant lesions and gastric epithelial polyps are commonly encountered in clinical practice. Surveillance of patients with premalignant gastric lesions may aid in early diagnosis of GC, and thus improve chances of survival. An expert professional workgroup was formed to summarise the current evidence and provide recommendations on the management of patients with gastric premalignant lesions in Singapore. Twenty-five recommendations were made to address screening and surveillance, strategies for detection and management of gastric premalignant lesions, management of gastric epithelial polyps, and pathological reporting of gastric premalignant lesions.

Published

2022

29. Safety and efficacy of an outpatient 12-step desensitization protocol for antineoplastic agents.

Author

Eroglu I, Filippova OT, Kirrane M, Orpen M, Almonte V, Thomas R, Lee-Teh M, Tizon R, Sklarin N, and O'Cearbhaill R

Abstract

Objective: Antineoplastic agents can cause hypersensitivity reactions that may preclude further treatment, possibly compromising patient outcome if the tumor remains sensitive to such agent. Although desensitization protocols can be used to re-introduce agents after the development of a hypersensitivity reaction, these protocols vary across institutions. Our study evaluated the safety and efficacy of our desensitization protocol., Methods: All patients who underwent desensitization to platinum, taxane, liposomal doxorubicin, or trastuzumab between November 2016 and May 2021 after a prior hypersensitivity reaction to the specific agent were included in a retrospective review. The 12-step, outpatient desensitization protocol included pretreatment with a leukotriene receptor antagonist, antihistamines, and corticosteroids, as well as extended infusion times. Successful desensitization was defined as the completion of ≥3 cycles without discontinuation of the agent due to a hypersensitivity reaction., Results: A total of 186 eligible patients were included. Median age was 59.5 years (range 26-87). 155 (83%) patients were treated with platinum. 55 (30%) patients were treated for colorectal cancer and 52 (28%) for ovarian cancer. 104 (56%) patients completed ≥3 cycles of therapy during desensitization. The median infusion time was 380 min (range 325-360 min). The median number of desensitization cycles was 3, with 694 cycles completed among all patients. A total of 79 (42%) patients had a breakthrough hypersensitivity reaction during desensitization, 4 of whom required epinephrine, and 84 (45%) patients discontinued the agent undergoing desensitization due to progression of disease., Conclusions: Our outpatient 12-step, institutional desensitization protocol for antineoplastic therapy proved safe and efficacious, with 56% of patients successfully completing ≥3 cycles and not requiring an inpatient admission., Competing Interests: Competing interests: REO reports personal fees from Tesaro/GSK, Regeneron, Seattle Genetics, Fresenius Kabi, the Gynecologic Oncology Foundation, Bayer, Immunogen, MJH Sciences and Curio, as well as others from AstraZeneca Pharmaceuticals (meal) and Hitech Health (travel). REO is also a non-compensated steering committee member for the PRIMA, Moonstone (Tesaro/GSK), DUO-O (AstraZeneca) studies, and Carina Biotech. Her institute receives funding for clinical research from Bayer/Celgene/Juno, Tesaro/GSK, Ludwig Cancer Institute, Abbvie/StemCentrx, Regeneron, TCR2 Therapeutics, Atara Biotherapeutics, MarkerTherapeutics, Syndax Pharmaceuticals, Genmab/Seagen Therapeutics, Sellas Therapeutics, Genentech, Kite Pharma, and the Gynecologic Oncology Foundation., (© IGCS and ESGO 2022. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2022

30. Severity of gastric intestinal metaplasia predicts the risk of gastric cancer: a prospective multicentre cohort study (GCEP).

Author

Lee JWJ, Zhu F, Srivastava S, Tsao SK, Khor C, Ho KY, Fock KM, Lim WC, Ang TL, Chow WC, So JBY, Koh CJ, Chua SJ, Wong ASY, Rao J, Lim LG, Ling KL, Chia CK, Ooi CJ, Rajnakova A, Yap WM, Salto-Tellez M, Ho B, Soong R, Chia KS, Teo YY, Teh M, and Yeoh KG

Subjects

Gastroscopy, Humans, Metaplasia, Prospective Studies, Risk Factors, Helicobacter Infections complications, Helicobacter Infections epidemiology, Helicobacter pylori, Precancerous Conditions epidemiology, Stomach Neoplasms diagnosis, Stomach Neoplasms epidemiology, Stomach Neoplasms etiology

Abstract

Objective: To investigate the incidence of gastric cancer (GC) attributed to gastric intestinal metaplasia (IM), and validate the Operative Link on Gastric Intestinal Metaplasia (OLGIM) for targeted endoscopic surveillance in regions with low-intermediate incidence of GC., Methods: A prospective, longitudinal and multicentre study was carried out in Singapore. The study participants comprised 2980 patients undergoing screening gastroscopy with standardised gastric mucosal sampling, from January 2004 and December 2010, with scheduled surveillance endoscopies at year 3 and 5. Participants were also matched against the National Registry of Diseases Office for missed diagnoses of early gastric neoplasia (EGN)., Results: There were 21 participants diagnosed with EGN. IM was a significant risk factor for EGN (adjusted-HR 5.36; 95% CI 1.51 to 19.0; p<0.01). The age-adjusted EGN incidence rates for patients with and without IM were 133.9 and 12.5 per 100 000 person-years. Participants with OLGIM stages III-IV were at greatest risk (adjusted-HR 20.7; 95% CI 5.04 to 85.6; p<0.01). More than half of the EGNs (n=4/7) attributed to baseline OLGIM III-IV developed within 2 years (range: 12.7-44.8 months). Serum trefoil factor 3 distinguishes (Area Under the Receiver Operating Characteristics 0.749) patients with OLGIM III-IV if they are negative for H. pylori . Participants with OLGIM II were also at significant risk of EGN (adjusted-HR 7.34; 95% CI 1.60 to 33.7; p=0.02). A significant smoking history further increases the risk of EGN among patients with OLGIM stages II-IV., Conclusions: We suggest a risk-stratified approach and recommend that high-risk patients (OLGIM III-IV) have endoscopic surveillance in 2 years, intermediate-risk patients (OLGIM II) in 5 years., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2022

31. A Cross-Sectional study on risk factors for severe hypoglycemia among Insulin-Treated elderly type 2 diabetes Mellitus (T2DM) patients in Singapore.

Author

Shi Min Ko M, Kit Lee W, Chang Ang L, Goh SY, Mong Bee Y, and Ming Teh M

Subjects

Aged, Blood Glucose, Cross-Sectional Studies, Glycated Hemoglobin analysis, Humans, Hypoglycemic Agents adverse effects, Insulin adverse effects, Risk Factors, Singapore epidemiology, Diabetes Mellitus, Type 2 chemically induced, Diabetes Mellitus, Type 2 drug therapy, Hypoglycemia chemically induced, Hypoglycemia epidemiology

Abstract

Objective: This study investigates the risk factors for severe hypoglycemia among Southeast Asian T2DM patients., Methods: Insulin-treated T2DM patients greater than 65 years old with HbA1c < 8% were recruited. They completed questionnaires detailing their experience of hypoglycemia and presence of impaired hypoglycemia awareness (IAH). Data on insulin treatment regimens, glycated haemoglobin (Hba1c) and comorbidities were also collected., Results: Of the 92 participants, 15.2% had at least one episode of severe hypoglycemia over the past year. Comparison between both groups showed that patients with severe hypoglycemia had lower Hba1c, higher Gold score (3.9 ± 1.9 vs. 2.5 ± 1.4; p < .05) and higher Hypoglycemia Fear Survey (HFS) worry score (39.1 ± 14.3 vs. 31.8 ± 11.8; p < .05). There were no significant differences in duration of diabetes and insulin treatment, treatment regimens and diabetes associated comorbidities except peripheral vascular disease. Furthermore, no significant differences were noted in HFS behavior score, hypoglycemia risk modifying behavior and social economic status., Conclusions: Patients with severe hypoglycemia had tighter glycemic control, greater IAH and higher worry scores regardless of treatment regimens. Clinicians may play a significant role in tightening glycemic control and influencing the risk of severe hypoglycemia. Standard structured diabetes education may help reduce the risk of severe hypoglycemia among this group of patients., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

32. Single-Cell Atlas of Lineage States, Tumor Microenvironment, and Subtype-Specific Expression Programs in Gastric Cancer.

Author

Kumar V, Ramnarayanan K, Sundar R, Padmanabhan N, Srivastava S, Koiwa M, Yasuda T, Koh V, Huang KK, Tay ST, Ho SWT, Tan ALK, Ishimoto T, Kim G, Shabbir A, Chen Q, Zhang B, Xu S, Lam KP, Lum HYJ, Teh M, Yong WP, So JBY, and Tan P

Subjects

Ecosystem, Humans, Single-Cell Analysis, Transcriptome, Tumor Microenvironment genetics, Cancer-Associated Fibroblasts pathology, Stomach Neoplasms genetics, Stomach Neoplasms pathology

Abstract

Gastric cancer heterogeneity represents a barrier to disease management. We generated a comprehensive single-cell atlas of gastric cancer (>200,000 cells) comprising 48 samples from 31 patients across clinical stages and histologic subtypes. We identified 34 distinct cell-lineage states including novel rare cell populations. Many lineage states exhibited distinct cancer-associated expression profiles, individually contributing to a combined tumor-wide molecular collage. We observed increased plasma cell proportions in diffuse-type tumors associated with epithelial-resident KLF2 and stage-wise accrual of cancer-associated fibroblast subpopulations marked by high INHBA and FAP coexpression. Single-cell comparisons between patient-derived organoids (PDO) and primary tumors highlighted inter- and intralineage similarities and differences, demarcating molecular boundaries of PDOs as experimental models. We complemented these findings by spatial transcriptomics, orthogonal validation in independent bulk RNA-sequencing cohorts, and functional demonstration using in vitro and in vivo models. Our results provide a high-resolution molecular resource of intra- and interpatient lineage states across distinct gastric cancer subtypes., Significance: We profiled gastric malignancies at single-cell resolution and identified increased plasma cell proportions as a novel feature of diffuse-type tumors. We also uncovered distinct cancer-associated fibroblast subtypes with INHBA-FAP-high cell populations as predictors of poor clinical prognosis. Our findings highlight potential origins of deregulated cell states in the gastric tumor ecosystem. This article is highlighted in the In This Issue feature, p. 587., (©2021 The Authors; Published by the American Association for Cancer Research.)

Published

2022

33. ISM1 protects lung homeostasis via cell-surface GRP78-mediated alveolar macrophage apoptosis.

Author

Lam TYW, Nguyen N, Peh HY, Shanmugasundaram M, Chandna R, Tee JH, Ong CB, Hossain MZ, Venugopal S, Zhang T, Xu S, Qiu T, Kong WT, Chakarov S, Srivastava S, Liao W, Kim JS, Teh M, Ginhoux F, Fred Wong WS, and Ge R

Subjects

Alveolar Epithelial Cells metabolism, Animals, Apoptosis immunology, Bronchoalveolar Lavage Fluid immunology, Disease Models, Animal, Endoplasmic Reticulum Chaperone BiP metabolism, Endoplasmic Reticulum Chaperone BiP physiology, Female, Homeostasis, Inflammation, Intercellular Signaling Peptides and Proteins physiology, Lung metabolism, Macrophages, Alveolar immunology, Macrophages, Alveolar physiology, Male, Mice, Mice, Inbred BALB C, Phagocytosis physiology, Pulmonary Disease, Chronic Obstructive metabolism, Pulmonary Emphysema metabolism, Smoke adverse effects, Smoking adverse effects, Nicotiana adverse effects, Intercellular Signaling Peptides and Proteins metabolism, Lung pathology, Macrophages, Alveolar metabolism

Abstract

Alveolar macrophages (AMs) are critical for lung immune defense and homeostasis. They are orchestrators of chronic obstructive pulmonary disease (COPD), with their number significantly increased and functions altered in COPD. However, it is unclear how AM number and function are controlled in a healthy lung and if changes in AMs without environmental assault are sufficient to trigger lung inflammation and COPD. We report here that absence of isthmin 1 (ISM1) in mice ( Ism1 -/- ) leads to increase in both AM number and functional heterogeneity, with enduring lung inflammation, progressive emphysema, and significant lung function decline, phenotypes similar to human COPD. We reveal that ISM1 is a lung resident anti-inflammatory protein that selectively triggers the apoptosis of AMs that harbor high levels of its receptor cell-surface GRP78 (csGRP78). csGRP78 is present at a heterogeneous level in the AMs of a healthy lung, but csGRP78 high AMs are expanded in Ism1 -/- mice, cigarette smoke (CS)-induced COPD mice, and human COPD lung, making these cells the prime targets of ISM1-mediated apoptosis. We show that csGRP78 high AMs mostly express MMP-12, hence proinflammatory. Intratracheal delivery of recombinant ISM1 (rISM1) depleted csGRP78 high AMs in both Ism1 -/- and CS-induced COPD mice, blocked emphysema development, and preserved lung function. Consistently, ISM1 expression in human lungs positively correlates with AM apoptosis, suggesting similar function of ISM1-csGRP78 in human lungs. Our findings reveal that AM apoptosis regulation is an important physiological mechanism for maintaining lung homeostasis and demonstrate the potential of pulmonary-delivered rISM1 to target csGRP78 as a therapeutic strategy for COPD., Competing Interests: Competing interest statement: R.G. is the scientific founder of NovoBreeze Therapeutics Co. Ltd, a private biopharma company., (Copyright © 2022 the Author(s). Published by PNAS.)

Published

2022

34. USPSTF2013 versus PLCOm2012 lung cancer screening eligibility criteria (International Lung Screening Trial): interim analysis of a prospective cohort study.

Author

Tammemägi MC, Ruparel M, Tremblay A, Myers R, Mayo J, Yee J, Atkar-Khattra S, Yuan R, Cressman S, English J, Bedard E, MacEachern P, Burrowes P, Quaife SL, Marshall H, Yang I, Bowman R, Passmore L, McWilliams A, Brims F, Lim KP, Mo L, Melsom S, Saffar B, Teh M, Sheehan R, Kuok Y, Manser R, Irving L, Steinfort D, McCusker M, Pascoe D, Fogarty P, Stone E, Lam DCL, Ng MY, Vardhanabhuti V, Berg CD, Hung RJ, Janes SM, Fong K, and Lam S

Subjects

Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Prospective Studies, Early Detection of Cancer, Lung Neoplasms diagnosis

Abstract

Background: Lung cancer is a major health problem. CT lung screening can reduce lung cancer mortality through early diagnosis by at least 20%. Screening high-risk individuals is most effective. Retrospective analyses suggest that identifying individuals for screening by accurate prediction models is more efficient than using categorical age-smoking criteria, such as the US Preventive Services Task Force (USPSTF) criteria. This study prospectively compared the effectiveness of the USPSTF2013 and PLCOm2012 model eligibility criteria., Methods: In this prospective cohort study, participants from the International Lung Screening Trial (ILST), aged 55-80 years, who were current or former smokers (ie, had ≥30 pack-years smoking history or ≤15 quit-years since last permanently quitting), and who met USPSTF2013 criteria or a PLCOm2012 risk threshold of at least 1·51% within 6 years of screening, were recruited from nine screening sites in Canada, Australia, Hong Kong, and the UK. After enrolment, patients were assessed with the USPSTF2013 criteria and the PLCOm2012 risk model with a threshold of at least 1·70% at 6 years. Data were collected locally and centralised. Main outcomes were the comparison of lung cancer detection rates and cumulative life expectancies in patients with lung cancer between USPSTF2013 criteria and the PLCOm2012 model. In this Article, we present data from an interim analysis. To estimate the incidence of lung cancers in individuals who were USPSTF2013-negative and had PLCOm2012 of less than 1·51% at 6 years, ever-smokers in the Prostate Lung Colorectal and Ovarian Cancer Screening Trial (PLCO) who met these criteria and their lung cancer incidence were applied to the ILST sample size for the mean follow-up occurring in the ILST. This trial is registered at ClinicalTrials.gov, NCT02871856. Study enrolment is almost complete., Findings: Between June 17, 2015, and Dec 29, 2020, 5819 participants from the International Lung Screening Trial (ILST) were enrolled on the basis of meeting USPSTF2013 criteria or the PLCOm2012 risk threshold of at least 1·51% at 6 years. The same number of individuals was selected for the PLCOm2012 model as for the USPSTF2013 criteria (4540 [78%] of 5819). After a mean follow-up of 2·3 years (SD 1·0), 135 lung cancers occurred in 4540 USPSTF2013-positive participants and 162 in 4540 participants included in the PLCOm2012 of at least 1·70% at 6 years group (cancer sensitivity difference 15·8%, 95% CI 10·7-22·1%; absolute odds ratio 4·00, 95% CI 1·89-9·44; p<0·0001). Compared to USPSTF2013-positive individuals, PLCOm2012-selected participants were older (mean age 65·7 years [SD 5·9] vs 63·3 years [5·7]; p<0·0001), had more comorbidities (median 2 [IQR 1-3] vs 1 [1-2]; p<0·0001), and shorter life expectancy (13·9 years [95% CI 12·8-14·9] vs 14·8 [13·6-16·0] years). Model-based difference in cumulative life expectancies for those diagnosed with lung cancer were higher in those who had PLCOm2012 risk of at least 1·70% at 6 years than individuals who were USPSTF2013-positive (2248·6 years [95% CI 2089·6-2425·9] vs 2000·7 years [1841·2-2160·3]; difference 247·9 years, p=0·015)., Interpretation: PLCOm2012 appears to be more efficient than the USPSTF2013 criteria for selecting individuals to enrol into lung cancer screening programmes and should be used for identifying high-risk individuals who benefit from the inclusion in these programmes., Funding: Terry Fox Research Institute, The UBC-VGH Hospital Foundation and the BC Cancer Foundation, the Alberta Cancer Foundation, the Australian National Health and Medical Research Council, Cancer Research UK and a consortium of funders, and the Roy Castle Lung Cancer Foundation for the UK Lung Screen Uptake Trial., Competing Interests: Declaration of interests MCT developed the PLCOm2012 lung cancer risk prediction models, which is used in this study. The model is open access and is available free of charge to non-commercial users. For commercial users, licensing has been assigned to Brock University. MCT has not received any money for use of the PLCOm2012 model and does not anticipate any payments in the future. AM received travel or accommodation support for meetings by Roche, Olympus, and the International Association for the Study of Lung Cancer. JE received travel or accommodation support for meetings by Terry Fox Research Institute. MR received travel support from Takeda and American Thoracic Society. KF received travel support from various medical or scientific meeting organisers for participating or being a speaker (or both) and received additional grants or contracts from Olympus and Australian MRFF Next Generation Clinical Researchers Program and MeVis Medical Solutions AG/HealthInc; and payment or honoraria for lectures, presentations, and speaker's bureaus from Willey Cochrane Clinical Answers and is the Chair for Lung Cancer Consultative Group (unpaid) and a Council member. AT received consultancy fees from Olympus Respiratory America and additional grants or contracts from Biodesix Inc and Arch Biomedical Inc. CDB received consultancy fees from Mercy BioAnalytics, Grail, and Lucid Diagnostics and participated on a data safety monitoring board or advisory board for the International Lung Screening Trial. MR, DP, and DS received payment or honoraria for lectures, presentations, and speaker's bureaus by AstraZeneca. DS further received payment or honoraria for lectures, presentations, and speaker's bureaus from Bronchus Medical. MR further received additional grants or contracts provided by Grail. SL is an expert advisor and chair for Pan-Canadian Lung Cancer Screening Network and the Canadian Partnership Against Cancer. All other authors declare no competing interests., (Copyright © 2022 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY-NC-ND 4.0 license. Published by Elsevier Ltd.. All rights reserved.)

Published

2022

35. Induction of Gastric Cancer by Successive Oncogenic Activation in the Corpus.

Author

Douchi D, Yamamura A, Matsuo J, Melissa Lim YH, Nuttonmanit N, Shimura M, Suda K, Chen S, Pang S, Kohu K, Abe T, Shioi G, Kim G, Shabbir A, Srivastava S, Unno M, Bok-Yan So J, Teh M, Yeoh KG, Chuang LSH, and Ito Y

Subjects

Animals, Cell Dedifferentiation, Cell Lineage, Cell Transformation, Neoplastic metabolism, Cell Transformation, Neoplastic pathology, Chief Cells, Gastric pathology, Gene Expression Regulation, Neoplastic, Genes, APC, Genetic Predisposition to Disease, Integrases metabolism, Luminescent Proteins genetics, Luminescent Proteins metabolism, Metaplasia, Mice, Inbred C57BL, Mice, Transgenic, Mutation, Pepsinogen C metabolism, Phenotype, Precancerous Conditions enzymology, Precancerous Conditions pathology, Proto-Oncogene Proteins p21(ras) metabolism, Stomach Neoplasms enzymology, Stomach Neoplasms pathology, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Red Fluorescent Protein, Mice, Cell Proliferation, Cell Transformation, Neoplastic genetics, Chief Cells, Gastric enzymology, Integrases genetics, Pepsinogen C genetics, Precancerous Conditions genetics, Proto-Oncogene Proteins p21(ras) genetics, Stomach Neoplasms genetics, Transcriptional Activation

Abstract

Background & Aims: Metaplasia and dysplasia in the corpus are reportedly derived from de-differentiation of chief cells. However, the cellular origin of metaplasia and cancer remained uncertain. Therefore, we investigated whether pepsinogen C (PGC) transcript-expressing cells represent the cellular origin of metaplasia and cancer using a novel Pgc-specific CreERT2 recombinase mouse model., Methods: We generated a Pgc-mCherry-IRES-CreERT2 (Pgc-CreERT2) knock-in mouse model. Pgc-CreERT2/ + and Rosa-EYFP mice were crossed to generate Pgc-CreERT2/Rosa-EYFP (Pgc-CreERT2/YFP) mice. Gastric tissues were collected, followed by lineage-tracing experiments and histologic and immunofluorescence staining. We further established Pgc-CreERT2;Kras G12D/+ mice and investigated whether PGC transcript-expressing cells are responsible for the precancerous state in gastric glands. To investigate cancer development from PGC transcript-expressing cells with activated Kras, inactivated Apc, and Trp53 signaling pathways, we crossed Pgc-CreERT2/ + mice with conditional Kras G12D , Apc flox , Trp53 flox mice., Results: Expectedly, mCherry mainly labeled chief cells in the Pgc-CreERT2 mice. However, mCherry was also detected throughout the neck cell and isthmal stem/progenitor regions, albeit at lower levels. In the Pgc-CreERT2;Kras G12D/+ mice, PGC transcript-expressing cells with Kras G12D/+ mutation presented pseudopyloric metaplasia. The early induction of proliferation at the isthmus may reflect the ability of isthmal progenitors to react rapidly to Pgc-driven Kras G12D/+ oncogenic mutation. Furthermore, Pgc-CreERT2;Kras G12D/+ ;Apc flox/flox mice presented intramucosal dysplasia/carcinoma and Pgc-CreERT2;Kras G12D/+ ;Apc flox/flox ;Trp53 flox/flox mice presented invasive and metastatic gastric carcinoma., Conclusions: The Pgc-CreERT2 knock-in mouse is an invaluable tool to study the effects of successive oncogenic activation in the mouse corpus. Time-course observations can be made regarding the responses of isthmal and chief cells to oncogenic insults. We can observe stomach-specific tumorigenesis from the beginning to metastatic development., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2021

36. Iqgap3-Ras axis drives stem cell proliferation in the stomach corpus during homoeostasis and repair.

Author

Matsuo J, Douchi D, Myint K, Mon NN, Yamamura A, Kohu K, Heng DL, Chen S, Mawan NA, Nuttonmanit N, Li Y, Srivastava S, Ho SWT, Lee NYS, Lee HK, Adachi M, Tamura A, Chen J, Yang H, Teh M, So JB, Yong WP, Tan P, Yeoh KG, Chuang LSH, Tsukita S, and Ito Y

Subjects

Animals, Biomarkers, Tumor metabolism, Cell Proliferation physiology, Disease Models, Animal, Gene Expression Profiling, Mice, Mice, Inbred C57BL, Mice, Inbred Strains, Stomach Neoplasms drug therapy, Tamoxifen toxicity, GTPase-Activating Proteins metabolism, Gastric Mucosa cytology, Homeostasis physiology, Stem Cells cytology, Stomach Neoplasms metabolism

Abstract

Objective: Tissue stem cells are central regulators of organ homoeostasis. We looked for a protein that is exclusively expressed and functionally involved in stem cell activity in rapidly proliferating isthmus stem cells in the stomach corpus., Design: We uncovered the specific expression of Iqgap3 in proliferating isthmus stem cells through immunofluorescence and in situ hybridisation. We performed lineage tracing and transcriptomic analysis of Iqgap3 +isthmus stem cells with the Iqgap3-2A-tdTomato mouse model. Depletion of Iqgap3 revealed its functional importance in maintenance and proliferation of stem cells. We further studied Iqgap3 expression and the associated gene expression changes during tissue repair after tamoxifen-induced damage. Immunohistochemistry revealed elevated expression of Iqgap3 in proliferating regions of gastric tumours from patient samples., Results: Iqgap3 is a highly specific marker of proliferating isthmus stem cells during homoeostasis. Iqgap3+isthmus stem cells give rise to major cell types of the corpus unit. Iqgap3 expression is essential for the maintenance of stem potential. The Ras pathway is a critical partner of Iqgap3 in promoting strong proliferation in isthmus stem cells. The robust induction of Iqgap3 expression following tissue damage indicates an active role for Iqgap3 in tissue regeneration., Conclusion: IQGAP3 is a major regulator of stomach epithelial tissue homoeostasis and repair. The upregulation of IQGAP3 in gastric cancer suggests that IQGAP3 plays an important role in cancer cell proliferation., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2021. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2021

37. Author Correction: Highly recurrent CBS epimutations in gastric cancer CpG island methylator phenotypes and inflammation.

Author

Padmanabhan N, Kyon HK, Boot A, Lim K, Srivastava S, Chen S, Wu Z, Lee HO, Mukundan VT, Chan C, Chan YK, Xuewen O, Pitt JJ, Isa ZFA, Xing M, Lee MH, Tan ALK, Ting SHW, Luftig MA, Kappei D, Kruger WD, Bian J, Ho YS, Teh M, Rozen SG, and Tan P

Published

2021

38. Highly recurrent CBS epimutations in gastric cancer CpG island methylator phenotypes and inflammation.

Author

Padmanabhan N, Kyon HK, Boot A, Lim K, Srivastava S, Chen S, Wu Z, Lee HO, Mukundan VT, Chan C, Chan YK, Xuewen O, Pitt JJ, Isa ZFA, Xing M, Lee MH, Tan ALK, Ting SHW, Luftig MA, Kappei D, Kruger WD, Bian J, Ho YS, Teh M, Rozen SG, and Tan P

Subjects

Animals, Cell Line, Tumor, Epithelial Cells metabolism, Epithelial Cells pathology, Gene Deletion, Humans, Intestines pathology, Metaplasia, Mice, Transgenic, Phenotype, Proteome metabolism, Transcriptome genetics, CpG Islands genetics, Cystathionine beta-Synthase genetics, DNA Methylation genetics, Inflammation genetics, Mutation genetics, Stomach Neoplasms genetics

Abstract

Background: CIMP (CpG island methylator phenotype) is an epigenetic molecular subtype, observed in multiple malignancies and associated with the epigenetic silencing of tumor suppressors. Currently, for most cancers including gastric cancer (GC), mechanisms underlying CIMP remain poorly understood. We sought to discover molecular contributors to CIMP in GC, by performing global DNA methylation, gene expression, and proteomics profiling across 14 gastric cell lines, followed by similar integrative analysis in 50 GC cell lines and 467 primary GCs., Results: We identify the cystathionine beta-synthase enzyme (CBS) as a highly recurrent target of epigenetic silencing in CIMP GC. Likewise, we show that CBS epimutations are significantly associated with CIMP in various other cancers, occurring even in premalignant gastroesophageal conditions and longitudinally linked to clinical persistence. Of note, CRISPR deletion of CBS in normal gastric epithelial cells induces widespread DNA methylation changes that overlap with primary GC CIMP patterns. Reflecting its metabolic role as a gatekeeper interlinking the methionine and homocysteine cycles, CBS loss in vitro also causes reductions in the anti-inflammatory gasotransmitter hydrogen sulfide (H 2 S), with concomitant increase in NF-κB activity. In a murine genetic model of CBS deficiency, preliminary data indicate upregulated immune-mediated transcriptional signatures in the stomach., Conclusions: Our results implicate CBS as a bi-faceted modifier of aberrant DNA methylation and inflammation in GC and highlights H 2 S donors as a potential new therapy for CBS-silenced lesions.

Published

2021

39. Deep Intramural Left Anterior Descending or Large Septal Artery?

Author

Rathore K, Teh M, and Newman M

Subjects

Humans, Coronary Vessels, Surgeons

Published

2021

40. Hepcidin-Mediated Hypoferremia Disrupts Immune Responses to Vaccination and Infection.

Author

Frost JN, Tan TK, Abbas M, Wideman SK, Bonadonna M, Stoffel NU, Wray K, Kronsteiner B, Smits G, Campagna DR, Duarte TL, Lopes JM, Shah A, Armitage AE, Arezes J, Lim PJ, Preston AE, Ahern D, Teh M, Naylor C, Salio M, Gileadi U, Andrews SC, Dunachie SJ, Zimmermann MB, van der Klis FRM, Cerundolo V, Bannard O, Draper SJ, Townsend ARM, Galy B, Fleming MD, Lewis MC, and Drakesmith H

Subjects

Animals, Hepcidins genetics, Humans, Immunity, Humoral, Iron, Mice, Mice, Inbred C57BL, Mice, Knockout, Swine, Vaccination, Iron Deficiencies, Iron Metabolism Disorders

Abstract

Background: How specific nutrients influence adaptive immunity is of broad interest. Iron deficiency is the most common micronutrient deficiency worldwide and imparts a significant burden of global disease; however, its effects on immunity remain unclear., Methods: We used a hepcidin mimetic and several genetic models to examine the effect of low iron availability on T cells in vitro and on immune responses to vaccines and viral infection in mice. We examined humoral immunity in human patients with raised hepcidin and low serum iron caused by mutant TMPRSS6 . We tested the effect of iron supplementation on vaccination-induced humoral immunity in piglets, a natural model of iron deficiency., Findings: We show that low serum iron (hypoferremia), caused by increased hepcidin, severely impairs effector and memory responses to immunizations. The intensified metabolism of activated lymphocytes requires the support of enhanced iron acquisition, which is facilitated by IRP1/2 and TFRC. Accordingly, providing extra iron improved the response to vaccination in hypoferremic mice and piglets, while conversely, hypoferremic humans with chronically increased hepcidin have reduced concentrations of antibodies specific for certain pathogens. Imposing hypoferremia blunted the T cell, B cell, and neutralizing antibody responses to influenza virus infection in mice, allowing the virus to persist and exacerbating lung inflammation and morbidity., Conclusions: Hypoferremia, a well-conserved physiological innate response to infection, can counteract the development of adaptive immunity. This nutrient trade-off is relevant for understanding and improving immune responses to infections and vaccines in the globally common contexts of iron deficiency and inflammatory disorders., Funding: Medical Research Council, UK., Competing Interests: H.D. has sat on the advisory board of Kymab, received research funding from Pfizer and La Jolla Pharmaceutical Company, and received honoraria from Pharmacosmos and Vifor. The other authors declare no competing interests., (© 2020 The Authors.)

Published

2021

41. WBP2 promotes gastric cancer cell migration via novel targeting of LATS2 kinase in the Hippo tumor suppressor pathway.

Author

Hum M, Tan HJ, Yang Y, Srivastava S, Teh M, and Lim YP

Subjects

Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Cell Line, Tumor, Cell Movement genetics, Cell Proliferation genetics, Cell Proliferation physiology, Humans, Immunoblotting, Immunohistochemistry, Protein Serine-Threonine Kinases genetics, Real-Time Polymerase Chain Reaction, Signal Transduction genetics, Signal Transduction physiology, Stomach Neoplasms genetics, Trans-Activators genetics, Tumor Suppressor Proteins genetics, Cell Movement physiology, Protein Serine-Threonine Kinases metabolism, Stomach Neoplasms metabolism, Trans-Activators metabolism, Tumor Suppressor Proteins metabolism

Abstract

Dysregulation of signaling pathways is responsible for many human diseases. The lack of understanding of the molecular etiology of gastric cancer (GC) poses a substantial challenge to the development of effective cancer therapy. To better understand the molecular mechanisms underlying the pathogenesis of GC, which will facilitate the identification and development of effective therapeutic approaches to improve patient outcomes, mass spectrometry-based phosphoproteomics analysis was performed to map the global molecular changes in GC. A total of 530 proteins with altered phosphorylation levels were detected across a panel of 15 normal and GC cell lines. WW domain-binding protein 2 (WBP2) was validated to be upregulated in a subset of GC cell lines. WBP2 is overexpressed in 61% cases of GC compared to non-cancer tissues and high WBP2 expression correlates with poor clinical outcomes. WBP2 was found to be required for GC cell migration but is dispensable for cell growth and proliferation. WBP2 knockdown increased p-LATS2 with a concomitant increase in p-YAP, resulting in the cytoplasmic retention of YAP and ultimately the inhibition of YAP/TEAD activity and downregulation of TEAD target genes--CTGF and CYR61. Importantly, the loss of LATS2 reversed the activation of Hippo pathway caused by WBP2 knockdown, indicating that WBP2 acts through LATS2 to exert its function on the Hippo pathway. Moreover, WBP2 interacted with LATS2 to inhibit its phosphorylation and activity. In conclusion, our study established a pivotal role for WBP2 in the promotion of GC cell migration via a novel mechanism that inactivates the Hippo pathway transducer LATS2., (© 2021 Federation of American Societies for Experimental Biology.)

Published

2021

42. DNA damage signalling as an anti-cancer barrier in gastric intestinal metaplasia.

Author

Krishnan V, Lim DXE, Hoang PM, Srivastava S, Matsuo J, Huang KK, Zhu F, Ho KY, So JBY, Khor C, Tsao S, Teh M, Fock KM, Ang TL, Jeyasekharan AD, Tan P, Yeoh KG, and Ito Y

Subjects

Biopsy methods, DNA Damage genetics, DNA Methylation, Female, Gene Expression Regulation, Neoplastic, Humans, Hyaluronan Receptors analysis, Male, Metaplasia genetics, Metaplasia pathology, Middle Aged, Mutation, Protective Factors, Signal Transduction, Gastric Mucosa pathology, Histones genetics, Minichromosome Maintenance Complex Component 2 genetics, MutL Protein Homolog 1 genetics, Rad52 DNA Repair and Recombination Protein genetics, Stomach Neoplasms genetics, Stomach Neoplasms pathology, Werner Syndrome Helicase genetics

Abstract

Objective: Intestinal metaplasia (IM) is a premalignant stage that poses a greater risk for subsequent gastric cancer (GC). However, factors regulating IM to GC progression remain unclear. Previously, activated DNA damage response (DDR) signalling factors were shown to engage tumour-suppressive networks in premalignant lesions. Here, we interrogate the relationship of DDR signalling to mutational accumulation in IM lesions., Design: IM biopsies were procured from the gastric cancer epidemiology programme, an endoscopic surveillance programme where biopsies have been subjected to (epi)genomic characterisation. IM samples were classified as genome-stable or genome-unstable based on their mutational burden/somatic copy-number alteration (CNA) profiles. Samples were probed for DDR signalling and cell proliferation, using the markers γH2AX and MCM2, respectively. The expression of the gastric stem cell marker, CD44v9, was also assessed. Tissue microarrays representing the GC progression spectrum were included., Results: MCM2-positivity increased during GC progression, while γH2AX-positivity showed modest increase from normal to gastritis and IM stages, with further increase in GC. γH2AX levels correlated with the extent of chronic inflammation. Interestingly, genome-stable IM lesions had higher γH2AX levels underscoring a protective anti-cancer role for DDR signalling. In contrast, genome-unstable IM lesions with higher mutational burden/CNAs had lower γH2AX levels, elevated CD44v9 expression and modest promoter hypermethylation of DNA repair genes WRN, MLH1 and RAD52 ., Conclusions: Our data suggest that IM lesions with active DDR will likely experience a longer latency at the premalignant state until additional hits that override DDR signalling clonally expand and promote progression. These observations provide insights on the factors governing IM progression., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2020

43. An LCM-based genomic analysis of SPEM, Gastric Cancer and Pyloric Gland Adenoma in an Asian cohort.

Author

Srivastava S, Huang KK, Rebbani K, Das K, Fazreen Z, Yeoh KG, Tan P, and Teh M

Subjects

Adenoma pathology, Humans, Laser Capture Microdissection, Metaplasia genetics, Metaplasia pathology, Mutation, Precancerous Conditions pathology, Retrospective Studies, Singapore, Stomach pathology, Stomach Diseases pathology, Stomach Neoplasms pathology, Adenoma genetics, Gastric Mucosa pathology, Precancerous Conditions genetics, Stomach Diseases genetics, Stomach Neoplasms genetics

Abstract

Spasmolytic polypeptide-expressing metaplasia (SPEM) and pyloric gland adenoma (PGA) in the stomach are metaplastic and neoplastic lesions, respectively, in which gastric body glands are replaced by pyloric glands. The aim of this study was to evaluate the genomic profile of SPEM and compare it with intestinal-type gastric cancer (GC) and PGA. Thirteen gastrectomies showing PGA with or without dysplasia, GC and SPEM were retrospectively selected. MUC5AC, MUC6, gastrin, and TFF2 IHC were performed. Lesions were subjected to laser capture microdissection followed by DNA extraction. Forty-three DNA samples were extracted from PGA without cytological dysplasia, PGA with low-grade and high-grade dysplasia and pyloric gland adenocarcinoma, GC, SPEM, and adjacent normal tissue from the body of the stomach and were subjected to exome sequencing for 49 genes that are commonly dysregulated in GC. Sanger sequencing was performed for confirmation. Twenty nonsynonymous mutations were identified in SPEM, and none of these were frameshifts or indels. PGA with or without cytological dysplasia showed a significantly higher number of mutations compared with SPEM. As cytological dysplasia increased from no dysplasia to dysplasia in PGA, the percentage of frameshift mutations, indels, and missense variations increased. Further missense or frameshift mutations were observed in the KRAS, APC, TP53, and CTNNB1 genes in the PGA group. In GC, mutations were observed in the TP53 gene (p.Arg248Gln). Missense mutations in the MUC5AC, KRAS, BRAF, and EZH2 genes were common between SPEM and GC. SPEM showed fewer genomic variations than GC and PGA, and was genomically distinct from the pyloric epithelium in PGA. Stepwise progression of PGA from PGA without dysplasia to PGA with dysplasia/adenocarcinoma was associated an increase in mutations. SPEM appears to be more genomically similar to GC than PGA.

Published

2020

44. Extracorporeal membrane oxygenation-supported percutaneous angioplasty of coronary button stenosis after aortic root replacement.

Author

Rathore K, Weightman W, Teh M, and Newman M

Subjects

Aged, Early Diagnosis, Female, Humans, Myocardial Ischemia diagnosis, Myocardial Ischemia surgery, Percutaneous Coronary Intervention, Postoperative Complications diagnosis, Reoperation, Treatment Outcome, Angioplasty, Aorta surgery, Aortic Valve Insufficiency surgery, Blood Vessel Prosthesis Implantation methods, Coronary Stenosis surgery, Extracorporeal Membrane Oxygenation methods, Postoperative Complications surgery

Abstract

Background and Aim: A 73-year-old female patient had right coronary button stenosis following aortic root replacement., Methods: Myocardial ischemia led to hemodynamic instability followed by cardiogenic shock, which was successfully managed using venoarterial extracorporeal membrane oxygenation-supported right coronary button angioplasty., Results and Conclusion: Although the incidence of such complications is low, it is a life-threatening event that requires prompt diagnosis and it may pose a challenging clinical scenario for the treating team., (© 2020 Wiley Periodicals LLC.)

Published

2020

45. Left Atrial Anastomosing Hemangioma Causing Recurrent Pericardial Effusion.

Author

Rathore K, Yussouf R, Teh M, Jindal S, Wong D, and Newman M

Subjects

Humans, Male, Middle Aged, Recurrence, Heart Atria, Heart Neoplasms complications, Hemangioma complications, Pericardial Effusion etiology

Abstract

We report an extremely rare tumor in an adult patient who presented with recurrent pericardial effusion. The mass was an extracardiac tumor on the left atrial roof, which was excised by open heart surgery. Histologic examination confirmed a cardiac anastomosing hemangioma., (Copyright © 2020 The Society of Thoracic Surgeons. Published by Elsevier Inc. All rights reserved.)

Published

2020

46. AQP5 enriches for stem cells and cancer origins in the distal stomach.

Author

Tan SH, Swathi Y, Tan S, Goh J, Seishima R, Murakami K, Oshima M, Tsuji T, Phuah P, Tan LT, Wong E, Fatehullah A, Sheng T, Ho SWT, Grabsch HI, Srivastava S, Teh M, Denil SLIJ, Mustafah S, Tan P, Shabbir A, So J, Yeoh KG, and Barker N

Subjects

Animals, Biomarkers metabolism, Humans, Mice, Neoplastic Stem Cells metabolism, Pylorus pathology, Receptors, G-Protein-Coupled metabolism, Wnt Signaling Pathway, Aquaporin 5 metabolism, Carcinogenesis pathology, Neoplastic Stem Cells pathology, Stomach pathology, Stomach Neoplasms pathology

Abstract

LGR5 marks resident adult epithelial stem cells at the gland base in the mouse pyloric stomach 1 , but the identity of the equivalent human stem cell population remains unknown owing to a lack of surface markers that facilitate its prospective isolation and validation. In mouse models of intestinal cancer, LGR5 + intestinal stem cells are major sources of cancer following hyperactivation of the WNT pathway 2 . However, the contribution of pyloric LGR5 + stem cells to gastric cancer following dysregulation of the WNT pathway-a frequent event in gastric cancer in humans 3 -is unknown. Here we use comparative profiling of LGR5 + stem cell populations along the mouse gastrointestinal tract to identify, and then functionally validate, the membrane protein AQP5 as a marker that enriches for mouse and human adult pyloric stem cells. We show that stem cells within the AQP5 + compartment are a source of WNT-driven, invasive gastric cancer in vivo, using newly generated Aqp5-creERT2 mouse models. Additionally, tumour-resident AQP5 + cells can selectively initiate organoid growth in vitro, which indicates that this population contains potential cancer stem cells. In humans, AQP5 is frequently expressed in primary intestinal and diffuse subtypes of gastric cancer (and in metastases of these subtypes), and often displays altered cellular localization compared with healthy tissue. These newly identified markers and mouse models will be an invaluable resource for deciphering the early formation of gastric cancer, and for isolating and characterizing human-stomach stem cells as a prerequisite for harnessing the regenerative-medicine potential of these cells in the clinic.

Published

2020

47. A Loss-of-Function Mutation in the Integrin Alpha L ( Itgal ) Gene Contributes to Susceptibility to Salmonella enterica Serovar Typhimurium Infection in Collaborative Cross Strain CC042.

Author

Zhang J, Teh M, Kim J, Eva MM, Cayrol R, Meade R, Nijnik A, Montagutelli X, Malo D, and Jaubert J

Subjects

Animals, Bacteremia immunology, Bacteremia pathology, Bacterial Load, Bone Marrow pathology, Disease Models, Animal, Genes, Lymphocyte Subsets immunology, Mice, Mice, Inbred C57BL, Salmonella Infections immunology, Salmonella Infections pathology, Serogroup, Spleen pathology, Survival Analysis, Thymus Gland pathology, Bacteremia genetics, CD11a Antigen deficiency, Genetic Predisposition to Disease, Loss of Function Mutation, Salmonella Infections genetics, Salmonella typhimurium growth & development

Abstract

Salmonella is an intracellular bacterium found in the gastrointestinal tract of mammalian, avian, and reptilian hosts. Mouse models have been extensively used to model in vivo distinct aspects of human Salmonella infections and have led to the identification of several host susceptibility genes. We have investigated the susceptibility of Collaborative Cross strains to intravenous infection with Salmonella enterica serovar Typhimurium as a model of human systemic invasive infection. In this model, strain CC042/GeniUnc (CC042) mice displayed extreme susceptibility with very high bacterial loads and mortality. CC042 mice showed lower spleen weights and decreased splenocyte numbers before and after infection, affecting mostly CD8 + T cells, B cells, and all myeloid cell populations, compared with control C57BL/6J mice. CC042 mice also had lower thymus weights with a reduced total number of thymocytes and double-negative and double-positive (CD4 + , CD8 + ) thymocytes compared to C57BL/6J mice. Analysis of bone marrow-resident hematopoietic progenitors showed a strong bias against lymphoid-primed multipotent progenitors. An F2 cross between CC042 and C57BL/6N mice identified two loci on chromosome 7 ( Stsl6 and Stsl7 ) associated with differences in bacterial loads. In the Stsl7 region, CC042 carried a loss-of-function variant, unique to this strain, in the integrin alpha L ( Itgal ) gene, the causative role of which was confirmed by a quantitative complementation test. Notably, Itgal loss of function increased the susceptibility to S. Typhimurium in a (C57BL/6J × CC042)F1 mouse background but not in a C57BL/6J mouse inbred background. These results further emphasize the utility of the Collaborative Cross to identify new host genetic variants controlling susceptibility to infections and improve our understanding of the function of the Itgal gene., (Copyright © 2019 American Society for Microbiology.)

Published

2019

48. The desmosomal cadherin desmoglein-3 acts as a keratinocyte anti-stress protein via suppression of p53.

Author

Rehman A, Cai Y, Hünefeld C, Jedličková H, Huang Y, Teck Teh M, Sharif Ahmad U, Uttagomol J, Wang Y, Kang A, Warnes G, Harwood C, Bergamaschi D, Kenneth Parkinson E, Röcken M, and Wan H

Subjects

Animals, Antibodies immunology, Caspase 3 metabolism, Cells, Cultured, Desmoglein 3 deficiency, Dogs, Humans, Leupeptins pharmacology, Mice, Pemphigus blood, Pemphigus immunology, Pemphigus pathology, Proteolysis, Skin metabolism, Desmoglein 3 metabolism, Desmosomes metabolism, Keratinocytes metabolism, Stress, Physiological, Tumor Suppressor Protein p53 metabolism

Abstract

Desmoglein-3 (Dsg3), the Pemphigus Vulgaris (PV) antigen (PVA), plays an essential role in keratinocyte cell-cell adhesion and regulates various signaling pathways involved in the progression and metastasis of cancer where it is upregulated. We show here that expression of Dsg3 impacts on the expression and function of p53, a key transcription factor governing the responses to cellular stress. Dsg3 depletion increased p53 expression and activity, an effect enhanced by treating cells with UVB, mechanical stress and genotoxic drugs, whilst increased Dsg3 expression resulted in the opposite effects. Such a pathway in the negative regulation of p53 by Dsg3 was Dsg3 specific since neither E-cadherin nor desmoplakin knockdown caused similar effects. Analysis of Dsg3 -/- mouse skin also indicated an increase of p53/p21 WAF1/CIP1 and cleaved caspase-3 relative to Dsg3 +/- controls. Finally, we evaluated whether this pathway was operational in the autoimmune disease PV in which Dsg3 serves as a major antigen involved in blistering pathogenesis. We uncovered increased p53 with diffuse cytoplasmic and/or nuclear staining in the oral mucosa of patients, including cells surrounding blisters and the pre-lesional regions. This finding was verified by in vitro studies where treatment of keratinocytes with PV sera, as well as a characterized pathogenic antibody specifically targeting Dsg3, evoked pronounced p53 expression and activity accompanied by disruption of cell-cell adhesion. Collectively, our findings suggest a novel role for Dsg3 as an anti-stress protein, via suppression of p53 function, and this pathway is disrupted in PV.

Published

2019

49. IgG4-Related Kidney Disease: A Curious Case of Interstitial Nephritis with Hypocomplementemia.

Author

Wong ETY, Lahiri M, Teh M, and Leo CCH

Abstract

IgG4-related kidney disease has been relatively newly recognized over the last two decades as a combination of an autoimmune and allergic disorder, with elevated serum IgG4 level and hypocomplementemia among its characteristic features. Here we report the case of a man with interstitial nephritis presenting with acute kidney injury and hypocomplementemia but normal serum IgG4 level and provide a literature review of IgG4-related kidney disease. This case highlights the importance of IgG4-related kidney disease as an important differential diagnosis in any patient presenting with a clinical syndrome mimicking acute interstitial nephritis with hypocomplementemia. A high index of suspicion with a low threshold for performing a native kidney biopsy would be paramount as patients do respond well to corticosteroid therapy.

Published

2019

50. Increased Aortic Arch Calcification and Cardiomegaly is Associated with Rapid Renal Progression and Increased Cardiovascular Mortality in Chronic Kidney Disease.

Author

Chen SC, Teh M, Huang JC, Wu PY, Chen CY, Tsai YC, Chiu YW, Chang JM, and Chen HC

Subjects

Aged, Biomarkers, Cardiomegaly diagnosis, Cause of Death, Disease Progression, Female, Heart Function Tests, Humans, Kidney Function Tests, Male, Middle Aged, Prognosis, Renal Insufficiency, Chronic diagnosis, Vascular Calcification diagnosis, Aorta, Thoracic pathology, Cardiomegaly etiology, Cardiomegaly mortality, Renal Insufficiency, Chronic complications, Vascular Calcification etiology, Vascular Calcification mortality

Abstract

Vascular calcification and cardiomegaly are highly prevalent in chronic kidney disease (CKD) patients. However, the association of the combination of aortic arch calcification (AoAC) and cardio-thoracic ratio (CTR) with clinical outcomes in patients with CKD is not well investigated. This study investigated whether the combination of AoAC and CTR is associated with poor clinical outcomes in CKD stages 3-5 patients. We enrolled 568 CKD patients, and AoAC and CTR were determined by chest radiography at enrollment. Rapid renal progression was defined as estimated glomerular filtration rate (eGFR) decline over 3 ml/min/1.73 m 2 per year. Both AoAC score and CTR were significantly associated with rapid renal progression. High CTR was correlated with increased risk for cardiovascular mortality. We stratified the patients into four groups according to the median AoAC score of 4 and CTR of 50%. Those with AoAC ≥ 4 and CTR ≥ 50% (vs. AoAC score < 4 and CTR < 50%) were associated with eGFR decline over 3 ml/min/1.73 m 2 /year and cardiovascular mortality. AoAC and CTR were independently associated with eGFR slope. In conclusion, the combination of increased AoAC and cardiomegaly was associated with rapid renal progression and increased cardiovascular mortality in patients with CKD stage 3-5 patients. We suggest that evaluating AoAC and CTR on chest plain radiography may be a simple and inexpensive method for detecting CKD patients at high risk for adverse clinical outcomes.

Published

2019