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1. Chameleon project: a children's end-of-life care quality improvement project.

Author

Wolff, Toni, Dorsett, Caroline, Connolly, Alexander, Kelly, Nicola, Turnbull, Jennifer, Deorukhkar, Anjum, Clements, Helena, Griffin, Hayley, Chhaochharia, Anjana, Haynes, Sarah, Webb, Kerry, and Manning, Joseph C

Subjects
Humans, Hospitalization, Terminal Care, Hospice Care, Child, State Medicine, Quality Improvement, length of stay, paediatrics, palliative Care, Pediatric, Clinical Research, Good Health and Well Being
Abstract

In response to there being no specialist paediatric palliative care (PPC) team in a region of England, we undertook a 12-month quality improvement project (funded by National Health Service England's Marginal Rate Emergency Threshold and Readmission fund) to improve children's end-of-life care.Improvements were implemented during two plan-do-study-act (PDSA) cycles and included specialist experts, clinical champions, focused education and training, and tools and materials to support identification, care planning and communication. A lead paediatrician with expertise in PPC (10 hours/week) led the project, supported by a PPC nurse (3 days/week) and a network administrator (2 days/week).Children who died an expected death were identified from the child death review teams. Numbers of non-elective hospital admissions, bed days, and costs were identified.Twenty-nine children died an expected death during the 12 months of the project and coincidentally 29 children died an expected death during the previous 12 months. The median number of non-elective admissions in the last 12 months of life was reduced from two per child to one. There was a reduction in specialist hospital (14%) and district general hospital (38%) bed days. The percentage of children who died an expected death who had anticipatory care plans rose from 50% to 72%.The results indicate that a network of clinicians with expertise in PPC working together across a region can improve personalised care planning and reduce admissions and bed days for children in their last year-of-life with reduced bed utilisation costs.

Published
2021

3. FGTD: Face Generation from Textual Description

Author

Deorukhkar, Kalpana, Kadamala, Kevlyn, Menezes, Elita, Kacprzyk, Janusz, Series Editor, Gomide, Fernando, Advisory Editor, Kaynak, Okyay, Advisory Editor, Liu, Derong, Advisory Editor, Pedrycz, Witold, Advisory Editor, Polycarpou, Marios M., Advisory Editor, Rudas, Imre J., Advisory Editor, Wang, Jun, Advisory Editor, Ranganathan, G., editor, Fernando, Xavier, editor, and Shi, Fuqian, editor

Published
2022
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7. Successful management of Methemoglobinemia and G6PD deficiency in a patient posted for surgical excision of branchial cyst

Author

V J Arun, Anuradha Deorukhkar, Aboobacker Mohamed Rafi, Deepak Charles, Rati Devendra, Susheela J Innah, and Prabhakar Kedar

Subjects
glucose-6-phosphate dehydrogenase, methemoglobinemia, novel mutation, Diseases of the blood and blood-forming organs, RC633-647.5
Abstract

A 27-year-old female patient who came for branchial cyst excision was found to have cyanosis and a saturation gap during preanesthetic check-up and hence she was referred to haematology for further workup. She had a Hb of 9 gm% with all other baseline tests as normal. Blood samples were sent for methaemoglobin estimation and related work up to the National Institute of Immunohematology (NIIH) Mumbai. She was diagnosed as a case of Methemoglobinemia with a methaemoglobin level of 68.7% with NADH cytochrome B5 reductase activity of 10.82 IU/g Hb. The drug of choice for treatment is Methylene blue and hence G6PD deficiency had to be ruled out prior to initiating therapy. She was found to have a concurrent existence of G6PD deficiency. The blood sample was further sent to NIIH for genetic confirmation. We avoided methylene blue and other precipitating factors that could trigger a haemolysis. She was further consulted by the Patient blood management team to optimize her erythropoiesis and avoid unnecessary transfusions. Anaesthetic consultation and planning were done to avoid drugs that could induce haemolysis. She was started on Vitamin C, Niacin, hematinic and advised to follow up after a month. She was symptomatically better. Cyanosis had reduced, and Hb improved to 12 gm%. She was taken up for surgery with all precautions. The surgery and the post-operative period were uneventful. She was discharged on postoperative day 4 with an advice to continue Vitamin C & Niacin and to follow-up in Haematology OPD after a month.

Published
2022
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8. Exploring the effect of Covid-19 on herding in Asian financial markets

Author

C.T. Vidya, Rashika Ravichandran, and Aditya Deorukhkar

Subjects
Cross-Sectional Absolute Deviation (CSAD), Science
Abstract

We examine herding behavior before, during, and after the Covid-19 pandemic in eight prominent Asian stock markets. Daily stock returns for the period Jan- 2018 to July- 2022 in the markets were investigated using the models prescribed by Chang et al., (2000) and Chiang and Zheng (2010). The empirical results provide strong support to earlier studies by providing robust evidence of herding in Vietnam, Indonesia, India, South Korea, and Singapore when the market is bullish and Indonesia and Vietnam also exhibit herding when the market is bearish. Herding tendency is dominant for Vietnam, India, and Indonesia during the pandemic with the post-pandemic time being more potent for China and Vietnam. Notably, an anti-herding tendency is found in China, Hong Kong, and Singapore. As a policy measure, efficient information dissemination, deterrence of insider trading, and regulation of mispricing can be undertaken.

Published
2023
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13. Polymer Nanocomposites

Author

Deorukhkar, Onkar A., primary, Radhakrishnan, S., additional, Munde, Yashwant S., additional, and Kulkarni, M. B., additional

Published
2021
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14. Chameleon project: a children’s end-of-life care quality improvement project

Author

Joseph C Manning, Hayley Griffin, Nicola Kelly, Sarah Haynes, Jennifer Turnbull, Helena Clements, Kerry Webb, Toni Wolff, Caroline Dorsett, Alexander Connolly, Anjum Deorukhkar, and Anjana Chhaochharia

Subjects
Medicine (General), R5-920
Abstract

In response to there being no specialist paediatric palliative care (PPC) team in a region of England, we undertook a 12-month quality improvement project (funded by National Health Service England’s Marginal Rate Emergency Threshold and Readmission fund) to improve children’s end-of-life care.Improvements were implemented during two plan–do–study–act (PDSA) cycles and included specialist experts, clinical champions, focused education and training, and tools and materials to support identification, care planning and communication. A lead paediatrician with expertise in PPC (10 hours/week) led the project, supported by a PPC nurse (3 days/week) and a network administrator (2 days/week).Children who died an expected death were identified from the child death review teams. Numbers of non-elective hospital admissions, bed days, and costs were identified.Twenty-nine children died an expected death during the 12 months of the project and coincidentally 29 children died an expected death during the previous 12 months. The median number of non-elective admissions in the last 12 months of life was reduced from two per child to one. There was a reduction in specialist hospital (14%) and district general hospital (38%) bed days. The percentage of children who died an expected death who had anticipatory care plans rose from 50% to 72%.The results indicate that a network of clinicians with expertise in PPC working together across a region can improve personalised care planning and reduce admissions and bed days for children in their last year-of-life with reduced bed utilisation costs.

Published
2021
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15. Reflective Assessments: Differentiation by Individualities

Author

Deorukhkar, Suneeta

Abstract

This article considers some aspects of the 'what, why and how' of individualising reflective assessments. It is an attempt to understand what works well in a special needs setting but it can also be applied within a mainstream context. The article comprises evidence, in the form of practitioner observations, during the author's work with eight students with complex, severe learning difficulties in a special needs school located in Greater London, as a part of a project called 'Brent Schools Reflective Writing'. Its findings, with an emphasis on developing independence amongst all SEND learners, support many of the recommendations contained in the final report of the Rochford Review (2013).

Published
2018
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20. Affordable Real-Time Heart Rate, ECG & SpO2 Monitoring System Using Internet of Things (IoT)

Author

Brendan Lucas, Aditya Mahamuni, Vinyas Kulal, Abhi Gupta, and Kalpana Deorukhkar

Subjects
General Medicine
Abstract

The healthcare industry now has an incomparable platform thanks to the Internet of Things technology, making it possible to quickly and effectively deal with challenges concerning healthcare. There has been a steady rise in the number of deaths due to sudden cardiac arrest (SCA) cases in developing countries and a lack of widespread use of an AED in these countries. The purpose of this study is to create an affordable Automated External Defibrillator (AED) that can be connected to IoT and can overcome certain drawbacks of the current AEDs. In the first phase of implementation, we attempt to create a Heart Monitoring System that can read Beats Per Minute (BPM), Electrocardiogram (ECG), and Saturation of Peripheral Oxygen (SpO2) using off-the-shelf sensors and display the data on a smartphone app. These sensors are connected to a Raspberry Pi 3b+, a single-board computer (SBC), which controls the entire system. The implementation of the system is successful, transmitting heart vitals to a smartphone app in real time. Further, the limitations of the system and future improvements are also discussed. The study builds a Heart Monitoring System under $67 with a few drawbacks. Further studies with better equipment are required to make the system accessible and less error-prone.

Published
2022

22. Stromal HIF2 Regulates Immune Suppression in the Pancreatic Cancer Microenvironment

Author

Carolina J. Garcia Garcia, Yanqing Huang, Natividad R. Fuentes, Madeleine C. Turner, Maria E. Monberg, Daniel Lin, Nicholas D. Nguyen, Tara N. Fujimoto, Jun Zhao, Jaewon J. Lee, Vincent Bernard, Meifang Yu, Abagail M. Delahoussaye, Iancarlos Jimenez Sacarello, Emily G. Caggiano, Jae L. Phan, Amit Deorukhkar, Jessica M. Molkentine, Dieter Saur, Anirban Maitra, and Cullen M. Taniguchi

Subjects
Immunosuppression Therapy, Pancreatic Neoplasms, Mice, Cancer-Associated Fibroblasts, Hepatology, Tumor Microenvironment, Gastroenterology, Animals, Humans, Hypoxia, Immune Checkpoint Inhibitors, Carcinoma, Pancreatic Ductal
Abstract

Pancreatic ductal adenocarcinoma (PDAC) has a hypoxic, immunosuppressive stroma that contributes to its resistance to immune checkpoint blockade therapies. The hypoxia-inducible factors (HIFs) mediate the cellular response to hypoxia, but their role within the PDAC tumor microenvironment remains unknown.We used a dual recombinase mouse model to delete Hif1α or Hif2α in α-smooth muscle actin-expressing cancer-associated fibroblasts (CAFs) arising within spontaneous pancreatic tumors. The effects of CAF HIF2α expression on tumor progression and composition of the tumor microenvironment were evaluated by Kaplan-Meier analysis, reverse transcription quantitative real-time polymerase chain reaction, histology, immunostaining, and by both bulk and single-cell RNA sequencing. CAF-macrophage crosstalk was modeled ex vivo using conditioned media from CAFs after treatment with hypoxia and PT2399, an HIF2 inhibitor currently in clinical trials. Syngeneic flank and orthotopic PDAC models were used to assess whether HIF2 inhibition improves response to immune checkpoint blockade.CAF-specific deletion of Hif2α, but not Hif1α, suppressed PDAC tumor progression and growth, and improved survival of mice by 50% (n = 21-23 mice/group, Log-rank P = .0009). Deletion of CAF-HIF2 modestly reduced tumor fibrosis and significantly decreased the intratumoral recruitment of immunosuppressive M2 macrophages and regulatory T cells. Treatment with the clinical HIF2 inhibitor PT2399 significantly reduced in vitro macrophage chemotaxis and M2 polarization, and improved tumor responses to immunotherapy in both syngeneic PDAC mouse models.Together, these data suggest that stromal HIF2 is an essential component of PDAC pathobiology and is a druggable therapeutic target that could relieve tumor microenvironment immunosuppression and enhance immune responses in this disease.

Published
2022

25. Data from Ursolic Acid Inhibits Growth and Metastasis of Human Colorectal Cancer in an Orthotopic Nude Mouse Model by Targeting Multiple Cell Signaling Pathways: Chemosensitization with Capecitabine

Author

Prasad, Sahdeo, primary, Yadav, Vivek R., primary, Sung, Bokyung, primary, Reuter, Simone, primary, Kannappan, Ramaswamy, primary, Deorukhkar, Amit, primary, Diagaradjane, Parmeswaran, primary, Wei, Caimiao, primary, Baladandayuthapani, Veerabhadran, primary, Krishnan, Sunil, primary, Guha, Sushovan, primary, and Aggarwal, Bharat B., primary

Published
2023
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26. Figure S5 from Selective EGLN Inhibition Enables Ablative Radiotherapy and Improves Survival in Unresectable Pancreatic Cancer

Author

Fujimoto, Tara N., primary, Colbert, Lauren E., primary, Huang, Yanqing, primary, Molkentine, Jessica M., primary, Deorukhkar, Amit, primary, Baseler, Laura, primary, de la Cruz Bonilla, Marimar, primary, Yu, Meifang, primary, Lin, Daniel, primary, Gupta, Sonal, primary, Cabeceiras, Peter K., primary, Kingsley, Charles V., primary, Tailor, Ramesh C., primary, Sawakuchi, Gabriel O., primary, Koay, Eugene J., primary, Piwnica-Worms, Helen, primary, Maitra, Anirban, primary, and Taniguchi, Cullen M., primary

Published
2023
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27. Data from Selective EGLN Inhibition Enables Ablative Radiotherapy and Improves Survival in Unresectable Pancreatic Cancer

Author

Fujimoto, Tara N., primary, Colbert, Lauren E., primary, Huang, Yanqing, primary, Molkentine, Jessica M., primary, Deorukhkar, Amit, primary, Baseler, Laura, primary, de la Cruz Bonilla, Marimar, primary, Yu, Meifang, primary, Lin, Daniel, primary, Gupta, Sonal, primary, Cabeceiras, Peter K., primary, Kingsley, Charles V., primary, Tailor, Ramesh C., primary, Sawakuchi, Gabriel O., primary, Koay, Eugene J., primary, Piwnica-Worms, Helen, primary, Maitra, Anirban, primary, and Taniguchi, Cullen M., primary

Published
2023
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28. Table S2 from Selective EGLN Inhibition Enables Ablative Radiotherapy and Improves Survival in Unresectable Pancreatic Cancer

Author

Fujimoto, Tara N., primary, Colbert, Lauren E., primary, Huang, Yanqing, primary, Molkentine, Jessica M., primary, Deorukhkar, Amit, primary, Baseler, Laura, primary, de la Cruz Bonilla, Marimar, primary, Yu, Meifang, primary, Lin, Daniel, primary, Gupta, Sonal, primary, Cabeceiras, Peter K., primary, Kingsley, Charles V., primary, Tailor, Ramesh C., primary, Sawakuchi, Gabriel O., primary, Koay, Eugene J., primary, Piwnica-Worms, Helen, primary, Maitra, Anirban, primary, and Taniguchi, Cullen M., primary

Published
2023
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29. Supplementary Figures S1-S3 from Imaging Epidermal Growth Factor Receptor Expression In vivo: Pharmacokinetic and Biodistribution Characterization of a Bioconjugated Quantum Dot Nanoprobe

Author

Diagaradjane, Parmeswaran, primary, Orenstein-Cardona, Jacobo M., primary, E. Colón-Casasnovas, Norman, primary, Deorukhkar, Amit, primary, Shentu, Shujun, primary, Kuno, Norihito, primary, Schwartz, David L., primary, Gelovani, Juri G., primary, and Krishnan, Sunil, primary

Published
2023
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30. Supplementary Data from A Novel Small-Molecule Inhibitor of Protein Kinase D Blocks Pancreatic Cancer Growth In vitro and In vivo

Author

Harikumar, Kuzhuvelil B., primary, Kunnumakkara, Ajaikumar B., primary, Ochi, Nobuo, primary, Tong, Zhimin, primary, Deorukhkar, Amit, primary, Sung, Bokyung, primary, Kelland, Lloyd, primary, Jamieson, Stephen, primary, Sutherland, Rachel, primary, Raynham, Tony, primary, Charles, Mark, primary, Bagherzadeh, Azadeh, primary, Foxton, Caroline, primary, Boakes, Alexandra, primary, Farooq, Muddasar, primary, Maru, Dipen, primary, Diagaradjane, Parmeswaran, primary, Matsuo, Yoichi, primary, Sinnett-Smith, James, primary, Gelovani, Juri, primary, Krishnan, Sunil, primary, Aggarwal, Bharat B., primary, Rozengurt, Enrique, primary, Ireson, Christopher R., primary, and Guha, Sushovan, primary

Published
2023
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31. Supplementary Table 1 from Ursolic Acid Inhibits Growth and Metastasis of Human Colorectal Cancer in an Orthotopic Nude Mouse Model by Targeting Multiple Cell Signaling Pathways: Chemosensitization with Capecitabine

Author

Prasad, Sahdeo, primary, Yadav, Vivek R., primary, Sung, Bokyung, primary, Reuter, Simone, primary, Kannappan, Ramaswamy, primary, Deorukhkar, Amit, primary, Diagaradjane, Parmeswaran, primary, Wei, Caimiao, primary, Baladandayuthapani, Veerabhadran, primary, Krishnan, Sunil, primary, Guha, Sushovan, primary, and Aggarwal, Bharat B., primary

Published
2023
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32. Supplementary Figure 1 from γ-Tocotrienol Inhibits Pancreatic Tumors and Sensitizes Them to Gemcitabine Treatment by Modulating the Inflammatory Microenvironment

Author

Kunnumakkara, Ajaikumar B., primary, Sung, Bokyung, primary, Ravindran, Jayaraj, primary, Diagaradjane, Parmeswaran, primary, Deorukhkar, Amit, primary, Dey, Sanjit, primary, Koca, Cemile, primary, Yadav, Vivek R., primary, Tong, Zhimin, primary, Gelovani, Juri G., primary, Guha, Sushovan, primary, Krishnan, Sunil, primary, and Aggarwal, Bharat B., primary

Published
2023
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33. Data from γ-Tocotrienol Inhibits Pancreatic Tumors and Sensitizes Them to Gemcitabine Treatment by Modulating the Inflammatory Microenvironment

Author

Kunnumakkara, Ajaikumar B., primary, Sung, Bokyung, primary, Ravindran, Jayaraj, primary, Diagaradjane, Parmeswaran, primary, Deorukhkar, Amit, primary, Dey, Sanjit, primary, Koca, Cemile, primary, Yadav, Vivek R., primary, Tong, Zhimin, primary, Gelovani, Juri G., primary, Guha, Sushovan, primary, Krishnan, Sunil, primary, and Aggarwal, Bharat B., primary

Published
2023
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34. Extensive Epidermal Skin Loss Secondary to HSV Type One: Neonatal Management Challenges

Author

Rebecca J Calthorpe, Emma Spencer, Jane C Ravenscroft, Ting S Tang, Anna E Martinez, and Anjum Deorukhkar

Subjects
Pediatrics, RJ1-570
Abstract

We describe a rare case of a preterm neonate presenting at birth with extensive epidermal skin loss of over 90% due to disseminated herpes simplex virus type one infection. Differential diagnosis included aplasia cutis and epidermolysis bullosa. Serum PCR and mouth swabs confirmed HSV type one, and the patient required three weeks of treatment with intravenous aciclovir, followed by oral aciclovir. We describe the management challenges and give practical solutions applicable to the care of a neonate presenting with widespread skin loss due to any aetiology.

Published
2019
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37. Data from A Novel Small-Molecule Inhibitor of Protein Kinase D Blocks Pancreatic Cancer Growth In vitro and In vivo

Author

Sushovan Guha, Christopher R. Ireson, Enrique Rozengurt, Bharat B. Aggarwal, Sunil Krishnan, Juri Gelovani, James Sinnett-Smith, Yoichi Matsuo, Parmeswaran Diagaradjane, Dipen Maru, Muddasar Farooq, Alexandra Boakes, Caroline Foxton, Azadeh Bagherzadeh, Mark Charles, Tony Raynham, Rachel Sutherland, Stephen Jamieson, Lloyd Kelland, Bokyung Sung, Amit Deorukhkar, Zhimin Tong, Nobuo Ochi, Ajaikumar B. Kunnumakkara, and Kuzhuvelil B. Harikumar

Abstract

Protein kinase D (PKD) family members are increasingly implicated in multiple normal and abnormal biological functions, including signaling pathways that promote mitogenesis in pancreatic cancer. However, nothing is known about the effects of targeting PKD in pancreatic cancer. Our PKD inhibitor discovery program identified CRT0066101 as a specific inhibitor of all PKD isoforms. The aim of our study was to determine the effects of CRT0066101 in pancreatic cancer. Initially, we showed that autophosphorylated PKD1 and PKD2 (activated PKD1/2) are significantly upregulated in pancreatic cancer and that PKD1/2 are expressed in multiple pancreatic cancer cell lines. Using Panc-1 as a model system, we showed that CRT0066101 reduced bromodeoxyuridine incorporation; increased apoptosis; blocked neurotensin-induced PKD1/2 activation; reduced neurotensin-induced, PKD-mediated Hsp27 phosphorylation; attenuated PKD1-mediated NF-κB activation; and abrogated the expression of NF-κB-dependent proliferative and prosurvival proteins. We showed that CRT0066101 given orally (80 mg/kg/d) for 24 days significantly abrogated pancreatic cancer growth in Panc-1 subcutaneous xenograft model. Activated PKD1/2 expression in the treated tumor explants was significantly inhibited with peak tumor concentration (12 μmol/L) of CRT0066101 achieved within 2 hours after oral administration. Further, we showed that CRT0066101 given orally (80 mg/kg/d) for 21 days in Panc-1 orthotopic model potently blocked tumor growth in vivo. CRT0066101 significantly reduced Ki-67–positive proliferation index (P < 0.01), increased terminal deoxynucleotidyl transferase–mediated dUTP nick end labeling–positive apoptotic cells (P < 0.05), and abrogated the expression of NF-κB–dependent proteins including cyclin D1, survivin, and cIAP-1. Our results show for the first time that a PKD-specific small-molecule inhibitor CRT0066101 blocks pancreatic cancer growth in vivo and show that PKD is a novel therapeutic target in pancreatic cancer. Mol Cancer Ther; 9(5); 1136–46. ©2010 AACR.

Published
2023

38. Data from Ursolic Acid Inhibits Growth and Metastasis of Human Colorectal Cancer in an Orthotopic Nude Mouse Model by Targeting Multiple Cell Signaling Pathways: Chemosensitization with Capecitabine

Author

Bharat B. Aggarwal, Sushovan Guha, Sunil Krishnan, Veerabhadran Baladandayuthapani, Caimiao Wei, Parmeswaran Diagaradjane, Amit Deorukhkar, Ramaswamy Kannappan, Simone Reuter, Bokyung Sung, Vivek R. Yadav, and Sahdeo Prasad

Abstract

Purpose: Development of chemoresistance, poor prognosis, and metastasis often renders the current treatments for colorectal cancer (CRC) ineffective. Whether ursolic acid, a component of numerous medicinal plants, either alone or in combination with capecitabine, can inhibit the growth and metastasis of human CRC was investigated.Experimental design: The effect of ursolic acid on proliferation of CRC cell lines was examined by mitochondrial dye uptake assay, apoptosis by esterase staining, NF-κB activation by DNA-binding assay, and protein expression by Western blot. The effect of ursolic acid on the growth and chemosensitization was also examined in orthotopically implanted CRC in nude mice.Results: We found that ursolic acid inhibited the proliferation of different colon cancer cell lines. This is correlated with inhibition of constitutive NF-κB activation and downregulation of cell survival (Bcl-xL, Bcl-2, cFLIP, and survivin), proliferative (cyclin D1), and metastatic (MMP-9, VEGF, and ICAM-1) proteins. When examined in an orthotopic nude mouse model, ursolic acid significantly inhibited tumor volume, ascites formation, and distant organ metastasis, and this effect was enhanced with capecitabine. Immunohistochemistry of tumor tissue indicated that ursolic acid downregulated biomarkers of proliferation (Ki-67) and microvessel density (CD31). This effect was accompanied by suppression of NF-κB, STAT3, and β-catenin. In addition, ursolic acid suppressed EGF receptor (EGFR) and induced p53 and p21 expression. We also observed bioavailability of ursolic acid in the serum and tissue of animals.Conclusion: Overall, our results show that ursolic acid can inhibit the growth and metastasis of CRC and further enhance the therapeutic effects of capecitabine through the suppression of multiple biomarkers linked to inflammation, proliferation, invasion, angiogenesis, and metastasis. Clin Cancer Res; 18(18); 4942–53. ©2012 AACR.

Published
2023

39. Data from Selective EGLN Inhibition Enables Ablative Radiotherapy and Improves Survival in Unresectable Pancreatic Cancer

Author

Cullen M. Taniguchi, Anirban Maitra, Helen Piwnica-Worms, Eugene J. Koay, Gabriel O. Sawakuchi, Ramesh C. Tailor, Charles V. Kingsley, Peter K. Cabeceiras, Sonal Gupta, Daniel Lin, Meifang Yu, Marimar de la Cruz Bonilla, Laura Baseler, Amit Deorukhkar, Jessica M. Molkentine, Yanqing Huang, Lauren E. Colbert, and Tara N. Fujimoto

Abstract

When pancreatic cancer cannot be removed surgically, patients frequently experience morbidity and death from progression of their primary tumor. Radiation therapy (RT) cannot yet substitute for an operation because radiation causes fatal bleeding and ulceration of the nearby stomach and intestines before achieving tumor control. There are no FDA-approved medications that prevent or reduce radiation-induced gastrointestinal injury. Here, we overcome this fundamental problem of anatomy and biology with the use of the oral EGLN inhibitor FG-4592, which selectively protects the intestinal tract from radiation toxicity without protecting tumors. A total of 70 KPC mice with autochthonous pancreatic tumors received oral FG-4592 or vehicle control ± ablative RT to a cumulative 75 Gy administered in 15 daily fractions to a limited tumor field. Although ablative RT reduced complications from local tumor progression, fatal gastrointestinal bleeding was observed in 56% of mice that received high-dose RT with vehicle control. However, radiation-induced bleeding was completely ameliorated in mice that received high-dose RT with FG-4592 (0% bleeding, P < 0.0001 compared with vehicle). Furthermore, FG-4592 reduced epithelial apoptosis by half (P = 0.002) and increased intestinal microvessel density by 80% compared with vehicle controls. EGLN inhibition did not stimulate cancer growth, as treatment with FG-4592 alone, or overexpression of HIF2 within KPC tumors independently improved survival. Thus, we provide a proof of concept for the selective protection of the intestinal tract by the EGLN inhibition to enable ablative doses of cytotoxic therapy in unresectable pancreatic cancer by reducing untoward morbidity and death from radiation-induced gastrointestinal bleeding.Significance:Selective protection of the intestinal tract by EGLN inhibition enables potentially definitive doses of radiation therapy. This might allow radiation to be a surgical surrogate for unresectable pancreatic cancer.

Published
2023

40. Figure S4 from Selective EGLN Inhibition Enables Ablative Radiotherapy and Improves Survival in Unresectable Pancreatic Cancer

Author

Cullen M. Taniguchi, Anirban Maitra, Helen Piwnica-Worms, Eugene J. Koay, Gabriel O. Sawakuchi, Ramesh C. Tailor, Charles V. Kingsley, Peter K. Cabeceiras, Sonal Gupta, Daniel Lin, Meifang Yu, Marimar de la Cruz Bonilla, Laura Baseler, Amit Deorukhkar, Jessica M. Molkentine, Yanqing Huang, Lauren E. Colbert, and Tara N. Fujimoto

Abstract

Figure S4. Metabolic cage analysis of mice treated with a clinically relevant course of dose-escalated RT to a limited upper abdominal field. (A) Water consumed during fractionated radiation treatments with area under the curve quantification in (B) (C) Food consumed during fractionated radiation treatments with area under the curve quantification in (D)

Published
2023

41. Supplementary Table 1 from Ursolic Acid Inhibits Growth and Metastasis of Human Colorectal Cancer in an Orthotopic Nude Mouse Model by Targeting Multiple Cell Signaling Pathways: Chemosensitization with Capecitabine

Author

Bharat B. Aggarwal, Sushovan Guha, Sunil Krishnan, Veerabhadran Baladandayuthapani, Caimiao Wei, Parmeswaran Diagaradjane, Amit Deorukhkar, Ramaswamy Kannappan, Simone Reuter, Bokyung Sung, Vivek R. Yadav, and Sahdeo Prasad

Abstract

PDF file, 52K, Assessment of synergistic drug combination treatments between ursolic acid and capecitabine.

Published
2023

42. Supplementary Figures S1-S3 from Imaging Epidermal Growth Factor Receptor Expression In vivo: Pharmacokinetic and Biodistribution Characterization of a Bioconjugated Quantum Dot Nanoprobe

Author

Sunil Krishnan, Juri G. Gelovani, David L. Schwartz, Norihito Kuno, Shujun Shentu, Amit Deorukhkar, Norman E. Colón-Casasnovas, Jacobo M. Orenstein-Cardona, and Parmeswaran Diagaradjane

Abstract

Supplementary Figures S1-S3 from Imaging Epidermal Growth Factor Receptor Expression In vivo: Pharmacokinetic and Biodistribution Characterization of a Bioconjugated Quantum Dot Nanoprobe

Published
2023

43. Table S1 from Selective EGLN Inhibition Enables Ablative Radiotherapy and Improves Survival in Unresectable Pancreatic Cancer

Author

Cullen M. Taniguchi, Anirban Maitra, Helen Piwnica-Worms, Eugene J. Koay, Gabriel O. Sawakuchi, Ramesh C. Tailor, Charles V. Kingsley, Peter K. Cabeceiras, Sonal Gupta, Daniel Lin, Meifang Yu, Marimar de la Cruz Bonilla, Laura Baseler, Amit Deorukhkar, Jessica M. Molkentine, Yanqing Huang, Lauren E. Colbert, and Tara N. Fujimoto

Abstract

Table S1. Distribution of Tumor and Treatment Characteristics for All Enrolled Animals by Treatment Group

Published
2023

44. Supplementary Data from A Novel Small-Molecule Inhibitor of Protein Kinase D Blocks Pancreatic Cancer Growth In vitro and In vivo

Author

Sushovan Guha, Christopher R. Ireson, Enrique Rozengurt, Bharat B. Aggarwal, Sunil Krishnan, Juri Gelovani, James Sinnett-Smith, Yoichi Matsuo, Parmeswaran Diagaradjane, Dipen Maru, Muddasar Farooq, Alexandra Boakes, Caroline Foxton, Azadeh Bagherzadeh, Mark Charles, Tony Raynham, Rachel Sutherland, Stephen Jamieson, Lloyd Kelland, Bokyung Sung, Amit Deorukhkar, Zhimin Tong, Nobuo Ochi, Ajaikumar B. Kunnumakkara, and Kuzhuvelil B. Harikumar

Abstract

Supplementary Data from A Novel Small-Molecule Inhibitor of Protein Kinase D Blocks Pancreatic Cancer Growth In vitro and In vivo

Published
2023

45. Data from Imaging Epidermal Growth Factor Receptor Expression In vivo: Pharmacokinetic and Biodistribution Characterization of a Bioconjugated Quantum Dot Nanoprobe

Author

Sunil Krishnan, Juri G. Gelovani, David L. Schwartz, Norihito Kuno, Shujun Shentu, Amit Deorukhkar, Norman E. Colón-Casasnovas, Jacobo M. Orenstein-Cardona, and Parmeswaran Diagaradjane

Abstract

Purpose: To develop and validate an optical imaging nanoprobe for the discrimination of epidermal growth factor (EGF) receptor (EGFR)–overexpressing tumors from surrounding normal tissues that also expresses EGFR.Experimental Design: Near-infrared (NIR) quantum dots (QD) were coupled to EGF using thiol-maleimide conjugation to create EGF-QD nanoprobes. In vitro binding affinity of these nanoprobes and unconjugated QDs was evaluated in a panel of cell lines, with and without anti-EGFR antibody pretreatment. Serial optical imaging of HCT116 xenograft tumors was done after systemic injection of QD and EGF-QD.Results: EGF-QD showed EGFR-specific binding in vitro. In vivo imaging showed three distinct phases, tumor influx (∼3 min), clearance (∼60 min), and accumulation (1-6 h), of EGF-QD nanoprobes. Both QD and EGF-QD showed comparable nonspecific rapid tumor influx and clearance followed by attainment of an apparent dynamic equilibrium at ∼60 min. Subsequently (1-6 h), whereas QD concentration gradually decreased in tumors, EGF-QDs progressively accumulated in tumors. On delayed imaging at 24 h, tumor fluorescence decreased to near-baseline levels for both QD and EGF-QD. Ex vivo whole-organ fluorescence, tissue homogenate fluorescence, and confocal microscopic analyses confirmed tumor-specific accumulation of EGF-QD at 4 h. Immunofluorescence images showed diffuse colocalization of EGF-QD fluorescence within EGFR-expressing tumor parenchyma compared with patchy perivascular sequestration of QD.Conclusion: These results represent the first pharmacokinetic characterization of a robust EGFR imaging nanoprobe. The measurable contrast enhancement of tumors 4 h after systemic administration of EGF-QD and its subsequent normalization at 24 h imply that this nanoprobe may permit quantifiable and repetitive imaging of EGFR expression.

Published
2023

46. Supplementary Figure 1 from γ-Tocotrienol Inhibits Pancreatic Tumors and Sensitizes Them to Gemcitabine Treatment by Modulating the Inflammatory Microenvironment

Author

Bharat B. Aggarwal, Sunil Krishnan, Sushovan Guha, Juri G. Gelovani, Zhimin Tong, Vivek R. Yadav, Cemile Koca, Sanjit Dey, Amit Deorukhkar, Parmeswaran Diagaradjane, Jayaraj Ravindran, Bokyung Sung, and Ajaikumar B. Kunnumakkara

Abstract

Supplementary Figure 1 from γ-Tocotrienol Inhibits Pancreatic Tumors and Sensitizes Them to Gemcitabine Treatment by Modulating the Inflammatory Microenvironment

Published
2023

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