Search

Your search keyword '"Green, Michael D."' showing total 30 results
Start Over Author "Green, Michael D." Publisher elsevier b.v.
30 results on '"Green, Michael D."'

4. Public reporting of black participation in anti-hypertensive drug clinical trials.

Author

Green, Michael D., Dalmage, Mahalia R., Lusk, Jay B., Kadhim, Emilie F., Skalla, Lesley A., and O'Brien, Emily C.

Abstract

Non-Hispanic Black people in the United States have the highest prevalence of essential hypertension. Unfortunately, clinical trials often underrepresent Black patients. We aim to understand whether trial sponsorship type is associated with representation of Black participants in anti-hypertensive drug clinical trials. Then, we contextualize our findings amongst current efforts to improve diversity in clinical research populations. We searched ClinicalTrials.gov in May 2022 for antihypertensive drug trials. Of n = 408 trials in our initial search, n = 97 (23.77%) met inclusion criteria and were stratified by sponsorship type (industry vs non-industry). Standardized tests of difference were employed to compare characteristics of these trials, and linear regression was used to model change over time. Of 97 trials reporting results from 2010 to 2020, there were minimal differences in the percent of Black patients enrolled in anti-hypertensive clinical trials by sponsorship type. Both industry and non-industry sponsored studies had high rates of non-reporting, with slightly more non-reporting for industry (73.2%) vs non-industry (66.67%) studies. Industry funded studies reported results to ClinicalTrials.gov within 23.3 ± 15.0 months from completing studies, while non-industry funded trials reported within 18.9 ± 10.8 months. Despite Black Americans carrying the highest burden of disease for essential hypertension, they are underrepresented in anti-hypertension clinical trials and their overall participation has decreased between 2010 and 2020. In addition, there is major underreporting of trial participant race. We implore researchers and funders to establish clear, meaningful targets for anti-hypertensive drug trial diversity, and improve transparency in reporting of study characteristics. [Display omitted] [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

5. Counterfeit anti-infective drugs

Author

Newton, Paul N., Green, Michael D., Fernandez, Facundo M., Day, Nicholas PJ, and White, Nicholas J.

Subjects
Drug resistance -- Analysis, Drug counterfeiting -- Analysis, Anti-infective agents -- Analysis, International cooperation -- Analysis
Published
2006

6. Harnessing the DNA Repair Pathway in Breast Cancer: Germline Mutations/Polymorphisms in Breast Radiation.

Author

Green, Michael D., Brenneman, Randall, Powell, Simon N., and Bergom, Carmen

Abstract

Molecular profiling facilitates opportunities for personalization of breast cancer management. Increasing availability of germline and somatic sequencing provides insight into predictors of treatment efficacy and treatment tolerance of patients with breast cancer. The presence of pathologic mutations can guide patient selection for breast conserving surgery vs mastectomy. However, our understanding of the interplay between genetic variants and radiotherapy responses and side effects remains incomplete. Here we review the available data on germline mutations and polymorphisms in breast cancer. We also outline their association with treatment tolerance, locoregional outcomes, and ongoing efforts to transform these insights into more effective treatment strategies in combination with radiotherapy. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

7. Cardiac Biomarkers Associated With Hospital Length of Stay After Pediatric Congenital Heart Surgery.

Author

Green, Michael D., Parker, Devin M., Everett, Allen D., Vricella, Luca, Jacobs, Marshall L., Jacobs, Jeffrey P., and Brown, Jeremiah R.

Abstract

Prolonged hospital length of stay after congenital heart surgery is a significant cost burden and is associated with postoperative morbidity. Our goal was to evaluate the association between pre- and postoperative biomarker levels and in-hospital length of stay for children after congenital heart surgery. We enrolled patients <18 years of age who underwent at least 1 congenital heart operation at Johns Hopkins Hospital from 2010 to 2014. Blood samples were collected before the index operation and at the end of the bypass. ST2 and N-terminal pro-brain natriuretic peptide (NT-proBNP) measurements were evaluated as log-transformed, median, and tercile cut-points. We evaluated the association between pre- and postoperative NT-proBNP and ST2 measurements with in-hospital postoperative length of stay using multivariate logistic regression. We adjusted for covariates used in The Society of Thoracic Surgeons Congenital Heart Surgery Mortality Risk Model. In our cohort 45% of our patients had an in-hospital postoperative length of stay longer than the median. Before adjustment preoperative NT-proBNP above the population median and the highest tercile exhibited a significantly longer in-hospital length of stay. After adjustment for covariates in the risk model, pre- and postoperative ST2 and NT-proBNP demonstrated a significantly longer length of stay. Perioperative ST2 and NT-proBNP had a significant association with increased postoperative in-hospital length of stay before and after adjustment. ST2 in particular could be used to guide an earlier assessment of patient risk for complications that may lead to adverse outcomes. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

9. Reversal of a neurologic paraneoplastic syndrome with octreotide (Sandostatin) in a patient with glucagonoma

Author

Holmes, Alex, Kilpatrick, Christine, Proietto, Joseph, and Green, Michael D.

Subjects
Paraneoplastic syndromes -- Drug therapy, Octreotide acetate -- Health aspects, Health, Health care industry
Abstract

The case history is presented of a 69-year-old female patient who developed diabetes mellitus and, several years later, metastatic pancreatic cancer. The diabetes was controlled with diet alone for eight years, then with glibenclamide, and insulin therapy was added after nine years. The patient developed diarrhea, dementia, leg weakness, and, ultimately, globally decreased cognitive function, visual changes, and profound weakness of the lower limbs. Exploratory surgery revealed, besides the tumor, sheets of glucagon-producing cells in the liver (glucagon is a hormone that increases the concentration of glucose in the blood). Treatment with a somatostatin analogue (a drug with similar actions to somatostatin) led to marked improvement of the patient's symptoms, and she was able to read and even walk again. The patient's symptoms were consistent with the glucagonoma syndrome, caused by excess production of glucagon by a tumor. In another report, a patient with a glucagonoma and dementia, optic atrophy, loss of balance, and lower limb weakness was described. It appears that a specific neurologic paraneoplastic syndrome (a condition affecting the nervous system in patients with cancer that cannot be attributed to the tumor or the tissue in which it is located) can be associated with glucagonomas. A circulating factor (probably not glucagon itself) may have caused the neurologic symptoms; somatostatin may have inhibited the production or action of that factor. Such a factor may be involved in other paraneoplastic neurologic syndromes. (Consumer Summary produced by Reliance Medical Information, Inc.)

Published
1991

10. Metabolism drives macrophage heterogeneity in the tumor microenvironment.

Author

Li, Shasha, Yu, Jiali, Huber, Amanda, Kryczek, Ilona, Wang, Zhuwen, Jiang, Long, Li, Xiong, Du, Wan, Li, Gaopeng, Wei, Shuang, Vatan, Linda, Szeliga, Wojciech, Chinnaiyan, Arul M., Green, Michael D., Cieslik, Marcin, and Zou, Weiping

Abstract

Tumor-associated macrophages (TAMs) are a major cellular component in the tumor microenvironment (TME). However, the relationship between the phenotype and metabolic pattern of TAMs remains poorly understood. We performed single-cell transcriptome profiling on hepatic TAMs from mice bearing liver metastatic tumors. We find that TAMs manifest high heterogeneity at the levels of transcription, development, metabolism, and function. Integrative analyses and validation experiments indicate that increased purine metabolism is a feature of TAMs with pro-tumor and terminal differentiation phenotypes. Like mouse TAMs, human TAMs are highly heterogeneous. Human TAMs with increased purine metabolism exhibit a pro-tumor phenotype and correlate with poor therapeutic efficacy to immune checkpoint blockade. Altogether, our work demonstrates that TAMs are developmentally, metabolically, and functionally heterogeneous and purine metabolism may be a key metabolic feature of a pro-tumor macrophage population. [Display omitted] • Single-cell RNA-seq reveals metabolic heterogeneity of TAMs • TAM metabolic patterns correlate with their functional features • Purine metabolism marks TAMs with pro-tumor and terminal phenotype • Purine metabolism signature correlates with patient outcome and response to ICB Li et al. examine the metabolic heterogeneity of tumor-associated macrophages (TAMs). They demonstrate metabolic patterns of TAMs correlate with their functional characteristics, and increased purine metabolism is a feature of TAMs with pro-tumor and terminal differentiation phenotype. They confirm these observations in patients with multiple types of cancer. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

11. Use of refractometry and colorimetry as field methods to rapidly assess antimalarial drug quality

Author

Green, Michael D., Nettey, Henry, Rojas, Ofelia Villalva, Pamanivong, Chansapha, Khounsaknalath, Lamphet, Ortiz, Miguel Grande, Newton, Paul N., Fernández, Facundo M., Vongsack, Latsamy, and Manolin, Ot

Subjects
*COLORIMETRIC analysis, *CLINICAL pharmacology, *ANTIMALARIALS, *CLINICAL drug trials
Abstract

Abstract: The proliferation of counterfeit and poor-quality drugs is a major public health problem; especially in developing countries lacking adequate resources to effectively monitor their prevalence. Simple and affordable field methods provide a practical means of rapidly monitoring drug quality in circumstances where more advanced techniques are not available. Therefore, we have evaluated refractometry, colorimetry and a technique combining both processes as simple and accurate field assays to rapidly test the quality of the commonly available antimalarial drugs; artesunate, chloroquine, quinine, and sulfadoxine. Method bias, sensitivity, specificity and accuracy relative to high-performance liquid chromatographic (HPLC) analysis of drugs collected in the Lao PDR were assessed for each technique. The HPLC method for each drug was evaluated in terms of assay variability and accuracy. The accuracy of the combined method ranged from 0.96 to 1.00 for artesunate tablets, chloroquine injectables, quinine capsules, and sulfadoxine tablets while the accuracy was 0.78 for enterically coated chloroquine tablets. These techniques provide a generally accurate, yet simple and affordable means to assess drug quality in resource-poor settings. [Copyright &y& Elsevier]

Published
2007
Full Text
View/download PDF

12. High-performance liquid chromatographic assay for the simultaneous determination of sulfadoxine and pyrimethamine from whole blood dried onto filter paper

Author

Green, Michael D., Mount, Dwight L., and Nettey, Henry

Subjects
*LIQUID chromatography, *BLOOD testing
Abstract

A method using solid-phase extraction and high-performance liquid chromatography is evaluated for the simultaneous determination of sulfadoxine and pyrimethamine from 0.1 ml of whole blood dried onto filter paper. Extraction recoveries are about 60% for both drugs. The coefficient of variation for intra-assay precision, inter-assay precision and accuracy is less than 10% for sulfadoxine (10–100 μg/ml) and pyrimethamine (1–10 μg/ml). [Copyright &y& Elsevier]

Published
2002
Full Text
View/download PDF

13. Effectiveness and safety of immune checkpoint inhibitors in Black patients versus White patients in a US national health system: a retrospective cohort study.

Author

Miller, Sean, Jiang, Ralph, Schipper, Matthew, Fritsche, Lars G, Strohbehn, Garth, Wallace, Beth, Brinzevich, Daria, Falvello, Virginia, McMahon, Benjamin H, Zamora-Resendiz, Rafael, Ramnath, Nithya, Dai, Xin, Sankar, Kamya, Edwards, Donna M, Allen, Steven G, Yoo, Shinjae, Crivelli, Silvia, Green, Michael D, and Bryant, Alex K

Subjects
*DRUG side effects, *BLACK people, *IMMUNE checkpoint inhibitors, *NON-small-cell lung carcinoma, *AFRICAN Americans
Abstract

Black patients were severely under-represented in the clinical trials that led to the approval of immune checkpoint inhibitors (ICIs) for all cancers. The aim of this study was to characterise the effectiveness and safety of ICIs in Black patients. We did a retrospective cohort study of patients in the US Veterans Health Administration (VHA) system's Corporate Data Warehouse containing electronic medical records for all patients who self-identified as non-Hispanic Black or African American (referred to as Black) or non-Hispanic White (referred to as White) and received PD-1, PD-L1, CTLA-4, or LAG-3 inhibitors between Jan 1, 2010, and Dec 31, 2023. Effectiveness outcomes were overall survival, time to treatment discontinuation, and time to next treatment. The safety outcome was the frequency of immune-related adverse events; assessed among a random sample of 1000 Black patients and 1000 White patients, 892 pairs were matched on the basis of baseline characteristics using 1:1 exact matching without replacement. After manual chart review, patients who did not receive ICI therapy or who had inadequate follow-up were excluded. The adjusted effect of race on each effectiveness outcome was assessed in the whole ICI-treated cohort with propensity-weighted Cox regression with robust standard errors. Immune-related adverse events outcomes were analysed in the random matched sample with multivariable Cox regression, adjusting for baseline characteristics. We identified 26 398 patients, of whom 4943 (18·7%) patients were Black, 21 455 (81·3%) were White, 895 (3·4%) were female, 25 503 (96·6%) were male, 11 859 (45%) had non-small-cell lung cancer, and 26 045 (98·7%) received PD-1 or PD-L1 inhibitors. As of data cutoff (Aug 28, 2024), median follow-up was 40·3 months (95% CI 38·3–42·3) for Black patients and 43·9 months (43·0–45·1) for White patients. Compared with White patients, Black patients had longer time to treatment discontinuation (2-year unadjusted rates 10·7% [95% CI 9·8–11·7] for Black patients vs 8·6% [8·2–9·0] for White patients; adjusted hazard ratio [HR] 0·91, 95% CI 0·87–0·95, p<0·0001), similar time to next treatment (23·5% [22·3–24·8] for Black patients vs 25·6% [25·0–26·2] for White patients; 1·00, 0·95–1·05, p=0·96), and slightly improved overall survival (36·5% [35·2–38·1] for Black patients vs 36·5% [35·8–37·1]; 0·95, 0·90–0·99, p=0·036). 1710 patients (n=862 Black and n=848 White) were analysed for safety outcomes. Compared with White patients, Black patients had a reduced risk of all-grade immune-related adverse events (unadjusted 2-year rate 33·1% [95% CI 28·9–37·1] vs 44·1% [95% CI 39·1–48·7]; adjusted HR 0·75, 95% CI 0·62–0·90, p=0·0026), immune-related adverse events requiring treatment with systemic steroids (0·61, 0·46–0·81, p=0·00051), and immune-related adverse events resulting in permanent ICI discontinuation (0·58, 0·44–0·78, p=0·00024). In exploratory analyses of irAE subtypes, a significant risk reduction in Black patients was found for colitis (0·46, 0·27–0·76, p=0·0026) and hyperthyroidism or hypothyroidism (0·63, 0·44–0·90, p=0·011), and no significant differences were found for any other immune-related adverse event subtypes analysed. Similar results were found in analyses using a steroid-based definition of immune-related adverse events among the entire ICI-treated cohort. Compared with White patients, Black patients had similar ICI effectiveness and lower toxicities among those treated in the national VHA system, potentially reflecting an important difference in the therapeutic ratio (ratio of benefit to harm) of ICIs. Our findings of decreased toxicity among Black patients require further investigation to assess their generalisability. Million Veteran Program, Office of Research and Development, Veterans Health Administration and the LUNGevity foundation. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

14. Impact of poor-quality medicines in the ‘developing’ world

Author

Newton, Paul N., Green, Michael D., and Fernández, Facundo M.

Subjects
*QUININE, *MEDICAL research, *ANTI-infective agents, *CINCHONA bark, *MEDICAL quality control, *PUBLIC health, *DECISION making, *THERAPEUTICS, DEVELOPING countries
Abstract

Since our ancestors began trading several millennia ago, counterfeit and substandard medicines have been a recurring problem, with history punctuated by crises in the supply of anti-microbials, such as fake cinchona bark in the 1600s and fake quinine in the 1800s. Unfortunately this problem persists, in particular afflicting unsuspecting patients in ‘developing’ countries. Poor-quality drugs are a vital (but neglected) public health problem. They contribute to a ‘crevasse’ between the enormous effort in therapeutic research and policy decisions and implementation of good-quality medicines. [Copyright &y& Elsevier]

Published
2010
Full Text
View/download PDF

15. Projected environmental and public health benefits of extended-interval dosing: an analysis of pembrolizumab use in a US national health system.

Author

Bryant, Alex K, Lewy, Jacqueline R, Bressler, R Daniel, Chopra, Zoey, Gyori, Derek J, Bazzell, Brian G, Moeller, Julie A, Jacobson, Sofia I, Fendrick, A Mark, Kerr, Eve A, Ramnath, Nithya, Green, Michael D, Hofer, Timothy P, Vaishnav, Parth, and Strohbehn, Garth W

Subjects
*GREENHOUSE gases, *ENVIRONMENTAL health, *PEMBROLIZUMAB, *CLIMATE change & health, *MEDICAL wastes
Abstract

Health care is a major source of greenhouse gas emissions, leading to climate change and public health harms. Changes are needed to improve the environmental sustainability of health-care practices, but such changes should not sacrifice patient outcomes or financial sustainability. Alternative dosing strategies that reduce the frequency with which specialty drugs are administered, without sacrificing patient outcomes, are an attractive possibility for improving environmental sustainability. We sought to inform environmentally sustainable cancer care by estimating and comparing the environmental and financial effects of alternative, clinically equivalent strategies for pembrolizumab administration. We conducted a retrospective analysis using a cohort of patients from the Veterans Health Administration (VHA) in the USA who received one or more pembrolizumab doses between May 1, 2020, and Sept 30, 2022. Using baseline, real-world administration of pembrolizumab, we generated simulated pembrolizumab use data under three near-equivalent counterfactual pembrolizumab administration strategies defined by combinations of weight-based dosing, pharmacy-level vial sharing and dose rounding, and extended-interval dosing (ie, every 6 weeks). For each counterfactual dosing strategy, we estimated greenhouse gas emissions related to pembrolizumab use across the VHA cohort using a deterministic environmental impact model that estimated greenhouse gas emissions due to patient travel, drug manufacture, and medical waste as the primary outcome measure. We identified 7813 veterans who received at least one dose of pembrolizumab-containing therapy in the VHA during the study period. 59 140 pembrolizumab administrations occurred in the study period, of which 46 255 (78·2%) were dosed at 200 mg every 3 weeks, 12 885 (21·8%) at 400 mg every 6 weeks, and 14 955 (25·3%) were coadministered with infusional chemotherapies. Adoption of weight-based, extended-interval pembrolizumab dosing (4 mg/kg every 6 weeks) and pharmacy-level stewardship strategies (ie, dose rounding and vial sharing) for all pembrolizumab infusions would have resulted in 24·7% fewer administration events than baseline dosing (44 533 events vs 59 140 events) and an estimated 200 metric tons less CO 2 emitted per year as a result of pembrolizumab use within the VHA (650 tons vs 850 tons of CO 2 , a relative reduction of 24%), largely due to reductions in distance travelled by patients to receive treatment. Similar results were observed when weight-based and extended-interval dosing were applied only to pembrolizumab monotherapy and pembrolizumab in combination with oral therapies. Alternative pembrolizumab administration strategies might have environmental advantages over the current dosing and compounding paradigms. Specialty medication dosing can be optimised for health-care spending and environmental sustainability without sacrificing clinical outcomes. None. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

16. Pneumonitis After Chemoradiotherapy and Adjuvant Durvalumab in Stage III Non-Small Cell Lung Cancer.

Author

Edwards, Donna M., Sankar, Kamya, Alseri, Aaren, Jiang, Ralph, Schipper, Matthew, Miller, Sean, Dess, Kathryn, Strohbehn, Garth W., Elliott, David A., Moghanaki, Drew, Ramnath, Nithya, Green, Michael D., and Bryant, Alex K.

Subjects
*NON-small-cell lung carcinoma, *PNEUMONIA, *CHEMORADIOTHERAPY, *VETERANS' health, *RECTAL cancer
Abstract

Adjuvant durvalumab after definitive chemoradiotherapy (CRT) for unresectable stage III non-small cell lung cancer (NSCLC) is well-tolerated in clinical trials. However, pneumonitis rates outside of clinical trials remain poorly defined with CRT followed by durvalumab. We aimed to describe the influence of durvalumab on pneumonitis rates among a large cohort of patients with stage III NSCLC. We studied patients with stage III NSCLC in the national Veterans Health Administration from 2015 to 2021 who received concurrent CRT alone or with adjuvant durvalumab. We defined pneumonitis as worsening respiratory symptoms with radiographic changes within 2 years of CRT and graded events according to National Cancer Institute Common Terminology Criteria for Adverse Events version 4.03. We used Cox regression to analyze risk factors for pneumonitis and the effect of postbaseline pneumonitis on overall survival. Among 1994 patients (989 CRT alone, 1005 CRT followed by adjuvant durvalumab), the 2-year incidence of grade 2 or higher pneumonitis was 13.9% for CRT alone versus 22.1% for CRT plus durvalumab (unadjusted P <.001). On multivariable analysis, durvalumab was associated with higher risk of grade 2 pneumonitis (hazard ratio, 1.45; 95% CI, 1.09-1.93; P =.012) but not grade 3 to 5 pneumonitis (P =.2). Grade 3 pneumonitis conferred worse overall survival (hazard ratio, 2.51; 95% CI, 2.06-3.05; P <.001) but grade 2 pneumonitis did not (P =.4). Adjuvant durvalumab use was associated with increased risk of low-grade but not higher-grade pneumonitis. Reassuringly, low-grade pneumonitis did not increase mortality risk. We observed increased rates of high-grade pneumonitis relative to clinical trials; the reasons for this require further study. [ABSTRACT FROM AUTHOR]

Published
2024
Full Text
View/download PDF

22. De-escalating adjuvant durvalumab treatment duration in stage III non-small cell lung cancer.

Author

Bryant, Alex K., Sankar, Kamya, Zhao, Lili, Strohbehn, Garth W., Elliott, David, Moghanaki, Drew, Kelley, Michael J., Ramnath, Nithya, and Green, Michael D.

Subjects
*THERAPEUTIC use of monoclonal antibodies, *LUNG cancer, *MONOCLONAL antibodies, *TREATMENT duration, *TUMOR classification, *COMPARATIVE studies, *CHEMORADIOTHERAPY, *DESCRIPTIVE statistics, *TERMINATION of treatment, *PROPORTIONAL hazards models
Abstract

One year of adjuvant durvalumab following concurrent chemoradiotherapy significantly improves progression-free survival (PFS) and overall survival (OS) for patients with stage III non-small cell lung cancer (NSCLC). However, the optimal length of adjuvant therapy has not been determined. We identified patients with stage III NSCLC treated with definitive chemoradiation and adjuvant durvalumab from November 2017 to April 2021 from the United States Veterans Affairs system. Predictors of early durvalumab discontinuation were evaluated with Cox proportional hazards regression. The effect of differing durations of durvalumab treatment (up to 6, 9, and 12 months) on PFS and OS were compared with a marginal structural model and time-dependent Cox modelling. We included 1006 patients with stage III non-small cell lung cancer who received concurrent chemoradiotherapy and at least one dose of adjuvant durvalumab. The median duration of durvalumab treatment was 7 months (interquartile range 2.8–11.5) and 31% completed the intended durvalumab course. The most common reasons for early discontinuation were tumour progression (22%), immune-related adverse events (15%), and non-immune-related toxicity (6.0%), Marginal structural models suggested similar PFS for 9 months versus 12 months of durvalumab treatment and inferior PFS for 6 months versus 12 months. A substantial proportion of patients undergoing adjuvant durvalumab discontinue therapy early due to toxicity, and shorter durvalumab treatment durations may provide similar disease control to 12 months of therapy. Prospective randomised controlled studies are needed to characterise the optimal durvalumab treatment duration in locally advanced NSCLC patients. • Real-world patients have higher durvalumab toxicity than in clinical trials. • Real-world patients receive fewer durvalumab cycles than in clinical trials. • Shorter adjuvant durvalumab durations may be equivalent to the current standard. • Shorter durvalumab durations may decrease cost and improve toxicity. • Prospective study of shorter durvalumab durations is warranted. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

23. Prognostic and Predictive Role of PD-L1 Expression in Stage III Non-small Cell Lung Cancer Treated With Definitive Chemoradiation and Adjuvant Durvalumab.

Author

Bryant, Alex K., Sankar, Kamya, Strohbehn, Garth W., Zhao, Lili, Daniel, Victoria, Elliott, David, Ramnath, Nithya, and Green, Michael D.

Subjects
*NON-small-cell lung carcinoma, *PROGRAMMED death-ligand 1, *CHEMORADIOTHERAPY
Abstract

Purpose: It is unclear whether programmed death ligand 1 (PD-L1) expression is prognostic or predictive of immunotherapy benefit among patients with stage III non-small cell lung cancer (NSCLC) treated with definitive chemoradiation and adjuvant durvalumab.Methods and Materials: We determined pretreatment tumor PD-L1 expression for 312 patients with stage III NSCLC treated with definitive chemoradiation and at least 1 dose of adjuvant durvalumab between November 2017 and April 2021 across the national Veterans Health Administration. Progression-free survival (PFS) and overall survival (OS) in PD-L1 expression subgroups (<1%, 1%-49%, and 50%-100%) were compared with 994 patients with stage III NSCLC treated without adjuvant durvalumab from 2015 to 2016.Results: PD-L1 expression was <1%, 1% to 49%, and 50% to 100% in 109 (34.9%), 96 (30.7%), and 107 (34.3%) patients, respectively. Increasing PD-L1 expression was associated with longer PFS (adjusted hazard ratio [aHR], 0.84 per 25% absolute increase in expression; 95% confidence interval [CI], 0.75-0.94; P = .003) and OS (aHR, 0.86 per 25% absolute increase in expression; 95% CI, 0.74-0.99; P = .036). Compared with the no-durvalumab group, PFS was longer for PD-L1 50% to 100% (aHR, 0.44; 95% CI, 0.32-0.60; P < .001) and PD-L1 1% to 49% (aHR, 0.64; 95% CI, 0.47-0.86; P = .003) but not PD-L1 <1% (aHR, 0.84; 95% CI, 0.64-1.10; P = .19). Similar results were found for OS, with no significant difference between the no-durvalumab group and PD-L1 <1% (aHR, 0.81; 95% CI, 0.58-1.13; P = .22).Conclusions: Increasing tumor PD-L1 expression is prognostic for PFS and OS among patients with stage III NSCLC treated with adjuvant durvalumab, and patients with PD-L1 expression <1% may have limited benefit from adjuvant durvalumab. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

24. Timing of Adjuvant Durvalumab Initiation Is Not Associated With Outcomes in Stage III Non-small Cell Lung Cancer.

Author

Bryant, Alex K., Sankar, Kamya, Strohbehn, Garth W., Zhao, Lili, Elliott, David, Daniel, Victoria, Ramnath, Nithya, and Green, Michael D.

Subjects
*NON-small-cell lung carcinoma, *DATABASE administration, *THERAPEUTIC use of monoclonal antibodies, *LUNG cancer, *LUNG tumors, *RETROSPECTIVE studies, *IMMUNOMODULATORS, *RESEARCH funding
Abstract

Purpose: It is unclear whether time from radiation therapy (RT) completion to durvalumab initiation influences the outcomes of stage III non-small cell lung cancer (NSCLC) treated with definitive chemoradiation and adjuvant durvalumab.Methods and Materials: Using the US Veterans Health Administration database, we retrospectively identified 728 patients with stage III NSCLC treated with definitive chemoradiation who started durvalumab within 120 days of radiation completion. Time between the last radiation treatment and first durvalumab infusion was analyzed in multivariable Cox regression models for the primary outcomes of progression-free survival (PFS) and overall survival (OS), adjusting for baseline patient and disease characteristics. The primary analysis used a 120-day landmark, measuring OS and PFS from 120 days after radiation completion.Results: Among 728 patients, the median time from RT completion to durvalumab start was 41 days (interquartile range 30-58). In multivariable Cox regression, time from RT completion to durvalumab start showed no association with PFS (adjusted hazard ratio [aHR] 1.01 per week, 95% confidence interval [CI] 0.98-1.04, P = .4) or OS (aHR 1.02 per week, 95% CI 0.98-1.06, P = .3). Starting durvalumab ≤14 days after RT was also not associated with improved PFS or OS. Results were robust in sensitivity analyses varying analytical technique.Conclusions: Timing of durvalumab initiation up to 120 days after RT completion is not associated with PFS or OS in this real-world patient cohort. [ABSTRACT FROM AUTHOR]

Published
2022
Full Text
View/download PDF

25. Translation of DNA Damage Response Inhibitors as Chemoradiation Sensitizers From the Laboratory to the Clinic.

Author

Parsels, Leslie A., Zhang, Qiang, Karnak, David, Parsels, Joshua D., Lam, Kwok, Willers, Henning, Green, Michael D., Rehemtulla, Alnawaz, Lawrence, Theodore S., and Morgan, Meredith A.

Subjects
*DNA repair, *DNA damage, *CHEMORADIOTHERAPY, *TREATMENT effectiveness, *LABORATORY mice, *TRANSLATING & interpreting
Abstract

Combination therapies with agents targeting the DNA damage response (DDR) offer an opportunity to selectively enhance the therapeutic index of chemoradiation or eliminate use of chemotherapy altogether. The successful translation of DDR inhibitors to clinical use requires investigating both their direct actions as (chemo)radiosensitizers and their potential to stimulate tumor immunogenicity. Beginning with high-throughput screening using both viability and DNA damage-reporter assays, followed by validation in gold-standard radiation colony-forming assays and in vitro assessment of mechanistic effects on the DDR, we describe proven strategies and methods leading to the clinical development of DDR inhibitors both with radiation alone and in combination with chemoradiation. Beyond these in vitro studies, we discuss the impact of key features of human xenograft and syngeneic mouse models on the relevance of in vivo tumor efficacy studies, particularly with regard to the immunogenic effects of combined therapy with radiation and DDR inhibitors. Finally, we describe recent technological advances in radiation delivery (using the small animal radiation research platform) that allow for conformal, clinically relevant radiation therapy in mouse models. This overall approach is critical to the successful clinical development and ultimate Food and Drug Administration approval of DDR inhibitors as (chemo)radiation sensitizers. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

26. Tim-4+ cavity-resident macrophages impair anti-tumor CD8+ T cell immunity.

Author

Chow, Andrew, Schad, Sara, Green, Michael D., Hellmann, Matthew D., Allaj, Viola, Ceglia, Nicholas, Zago, Giulia, Shah, Nisargbhai S., Sharma, Sai Kiran, Mattar, Marissa, Chan, Joseph, Rizvi, Hira, Zhong, Hong, Liu, Cailian, Bykov, Yonina, Zamarin, Dmitriy, Shi, Hongyu, Budhu, Sadna, Wohlhieter, Corrin, and Uddin, Fathema

Subjects
*MACROPHAGES, *IMMUNE checkpoint proteins, *ASCITIC fluids, *T cells, *CELL physiology, *TREATMENT effectiveness, *PERITONEAL macrophages, *CYTOTOXIC T cells
Abstract

Immune checkpoint blockade (ICB) has been a remarkable clinical advance for cancer; however, the majority of patients do not respond to ICB therapy. We show that metastatic disease in the pleural and peritoneal cavities is associated with poor clinical outcomes after ICB therapy. Cavity-resident macrophages express high levels of Tim-4, a receptor for phosphatidylserine (PS), and this is associated with reduced numbers of CD8+ T cells with tumor-reactive features in pleural effusions and peritoneal ascites from patients with cancer. We mechanistically demonstrate that viable and cytotoxic anti-tumor CD8+ T cells upregulate PS and this renders them susceptible to sequestration away from tumor targets and proliferation suppression by Tim-4+ macrophages. Tim-4 blockade abrogates this sequestration and proliferation suppression and enhances anti-tumor efficacy in models of anti-PD-1 therapy and adoptive T cell therapy in mice. Thus, Tim-4+ cavity-resident macrophages limit the efficacy of immunotherapies in these microenvironments. [Display omitted] • Metastatic involvement of the serous body cavities portends worse ICB outcomes • Tim-4 levels on human macrophages correlate with reduced CD8+ CD39+ T cells • Tim-4+ macrophages sequester and impair proliferation of CD8+ T cells • Tim-4 blockade enhances the efficacy of ICB and adoptive T cell therapy in mice Chow et al. demonstrate that metastatic involvement of the pleural and peritoneal cavities is associated with poor ICB efficacy in patients with cancer. Tim-4+ cavity-resident macrophages directly impair CD8 T cell function, and Tim-4 blockade enhances the efficacy of ICB and adoptive T cell therapy in mice. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

27. KDIGO clinical practice guideline for the care of kidney transplant recipients: a summary.

Author

Kasiske, Bertram L., Zeier, Martin G., Chapman, Jeremy R., Craig, Jonathan C., Ekberg, Henrik, Garvey, Catherine A., Green, Michael D., Jha, Vivekanand, Josephson, Michelle A., Kiberd, Bryce A., Kreis, Henri A., McDonald, Ruth A., Newmann, John M., Obrador, Gregorio T., Vincenti, Flavio G., Cheung, Michael, Earley, Amy, Raman, Gowri, Abariga, Samuel, and Wagner, Martin

Subjects
*DISEASE management, *KIDNEY transplantation, *IMMUNOSUPPRESSION, *CARDIOVASCULAR diseases, *CANCER
Abstract

The 2009 Kidney Disease: Improving Global Outcomes (KDIGO) clinical practice guideline on the monitoring, management, and treatment of kidney transplant recipients is intended to assist the practitioner caring for adults and children after kidney transplantation. The guideline development process followed an evidence-based approach, and management recommendations are based on systematic reviews of relevant treatment trials. Critical appraisal of the quality of the evidence and the strength of recommendations followed the Grades of Recommendation Assessment, Development, and Evaluation (GRADE) approach. The guideline makes recommendations for immunosuppression and graft monitoring, as well as prevention and treatment of infection, cardiovascular disease, malignancy, and other complications that are common in kidney transplant recipients, including hematological and bone disorders. Limitations of the evidence, especially the lack of definitive clinical outcome trials, are discussed and suggestions are provided for future research. This summary includes a brief description of methodology and the complete guideline recommendations but does not include the rationale and references for each recommendation, which are published elsewhere. [ABSTRACT FROM AUTHOR]

Published
2010
Full Text
View/download PDF

28. Detecting counterfeit antimalarial tablets by near-infrared spectroscopy

Author

Dowell, Floyd E., Maghirang, Elizabeth B., Fernandez, Facundo M., Newton, Paul N., and Green, Michael D.

Subjects
*ANTIMALARIALS, *FRAUD, *SPECTRUM analysis, DEVELOPING countries
Abstract

Abstract: Counterfeit antimalarial drugs are found in many developing countries, but it is challenging to differentiate between genuine and fakes due to their increasing sophistication. Near-infrared spectroscopy (NIRS) is a powerful tool in pharmaceutical forensics, and we tested this technique for discriminating between counterfeit and genuine artesunate antimalarial tablets. Using NIRS, we found that artesunate tablets could be identified as genuine or counterfeit with high accuracy. Multivariate classification models indicated that this discriminatory ability was based, at least partly, on the presence or absence of spectral signatures related to artesunate. This technique can be field-portable and requires little training after calibrations are developed, thus showing great promise for rapid and accurate fake detection. [Copyright &y& Elsevier]

Published
2008
Full Text
View/download PDF

29. Characterization of outcomes in patients with advanced genitourinary malignancies treated with immune checkpoint inhibitors.

Author

Ma, Vincent T., Su, Christopher T., Hu, Miriam, Taylor, Jeremy M.G., Daignault-Newton, Stephanie, Kellezi, Olesia, Dahl, Megan N., Shah, Miloni A., Erickson, Stephanie, Lora, Jessica, Hamasha, Reema, Ali, Alicia, Yancey, Sabrina, Kiros, Leah, Balicki, Hannah M., Winfield, Daniel C., Green, Michael D., and Alva, Ajjai S.

Subjects
*IMMUNE checkpoint inhibitors, *DRUG side effects, *PROPORTIONAL hazards models, *OVERALL survival, *RENAL cell carcinoma, *IPILIMUMAB
Abstract

Purpose: Several immune checkpoint inhibitors (ICIs) are FDA approved for treatment of genitourinary (GU) malignancies. We aim to determine demographic and clinicopathologic characteristics that significantly affect clinical outcomes in patients with advanced stage GU malignancies treated with ICIs.Materials and Methods: We performed a single-center, consecutive, retrospective cohort analysis on patients with metastatic or unresectable GU malignancies who were treated with ICIs at the University of Michigan. Immune-related adverse events (irAEs), putative immune-mediated allergies, and overall response rates (ORR) were assessed. Comorbidity index scores were calculated. Survival analysis was performed to evaluate progression-free survival (PFS) and overall survival (OS), stratifying and controlling for a variety of clinicopathologic baseline factors including site of metastases.Results: A total of 160 patients were identified with advanced renal cell carcinoma (RCC) or urothelial carcinoma. Median PFS and OS were 5.0 and 23.6 months for RCC, and 2.8 and 9.6 months for urothelial carcinoma, respectively. Patients who experienced increased frequency and higher grade irAEs had better ICI treatment response (P < 0.0001). Presence of liver metastases was associated with poor response to ICI therapy (P = 0.001). Multivariable modeling demonstrates that patients with urothelial carcinoma and liver metastases had statistically worse PFS and OS compared to patients with RCC or other sites of metastases, respectively.Conclusion: Greater frequency and higher grades of irAEs are associated with better treatment response in patients with RCC and urothelial malignancy receiving ICI therapy. The presence of liver metastases denotes a negative predictive marker for immunotherapy efficacy.Summary: Immune checkpoint inhibitors (ICI) are increasingly used to treat genitourinary (GU) malignancies. However, clinical data regarding patients with advanced-stage GU malignancies treated with ICI is lacking. Thus, we performed a single-center, retrospective cohort study on patients with metastatic and unresectable renal cell carcinoma (RCC) and urothelial carcinoma who were treated with ICIs at the University of Michigan to provide demographic and clinicopathologic data regarding this population. We specifically focused on immune-related adverse events (irAEs), immune-mediated allergies, and the associated overall response rates (ORR). To better assess performance status, we calculated comorbidity scores for all patients. Finally, survival analyses for progression-free survival (PFS) and overall survival (OS) were performed using Kaplan-Meier analysis and Cox proportional hazards modeling, stratifying and controlling for clinicopathologic baseline factors, including sites of metastases, in our multivariable analysis. A total of 160 patients were identified with advanced RCC or urothelial carcinoma. We found decreased PFS (2.8 vs. 5.0 months) and decreased OS (9.8 vs. 23.6 months) for urothelial carcinoma compared to RCC patients. We noted that patients who experienced increased frequency and higher grades of irAEs had better treatment ORR with ICI therapy (P ≤ 0.0001). The presence of liver metastases was associated with worse ORR (P = 0.001), PFS (P = 0.0014), and OS (P = 0.0028) compared to other sites of metastases including lymph node, lung, and CNS/bone. The poor PFS and OS associated with urothelial carcinoma and liver metastases were preserved in our multivariable modeling after controlling for pertinent clinical factors. We conclude that greater frequency and higher grades of irAEs are associated with better treatment response in GU malignancy patients receiving ICI, a finding that is consistent with published studies in other cancers. The presence of liver metastases represents a significantly poor predictive marker in GU malignancy treated with ICI. Our findings contribute to the growing body of literature that seeks to understand the clinicopathologic variables and outcomes associated with ICI therapy. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

30. Stanniocalcin 1 is a phagocytosis checkpoint driving tumor immune resistance.

Author

Lin, Heng, Kryczek, Ilona, Li, Shasha, Green, Michael D., Ali, Alicia, Hamasha, Reema, Wei, Shuang, Vatan, Linda, Szeliga, Wojciech, Grove, Sara, Li, Xiong, Li, Jing, Wang, Weichao, Yan, Yijian, Choi, Jae Eun, Li, Gaopeng, Bian, Yingjie, Xu, Ying, Zhou, Jiajia, and Yu, Jiali

Subjects
*PHAGOCYTOSIS, *ANTIGEN presentation, *DENDRITIC cells, *T cells, *CANCER invasiveness, *CALRETICULIN
Abstract

Immunotherapy induces durable clinical responses in a fraction of patients with cancer. However, therapeutic resistance poses a major challenge to current immunotherapies. Here, we identify that expression of tumor stanniocalcin 1 (STC1) correlates with immunotherapy efficacy and is negatively associated with patient survival across diverse cancer types. Gain- and loss-of-function experiments demonstrate that tumor STC1 supports tumor progression and enables tumor resistance to checkpoint blockade in murine tumor models. Mechanistically, tumor STC1 interacts with calreticulin (CRT), an "eat-me" signal, and minimizes CRT membrane exposure, thereby abrogating membrane CRT-directed phagocytosis by antigen-presenting cells (APCs), including macrophages and dendritic cells. Consequently, this impairs APC capacity of antigen presentation and T cell activation. Thus, tumor STC1 inhibits APC phagocytosis and contributes to tumor immune evasion and immunotherapy resistance. We suggest that STC1 is a previously unappreciated phagocytosis checkpoint and targeting STC1 and its interaction with CRT may sensitize to cancer immunotherapy. [Display omitted] • Tumor STC1 negatively correlates with immunotherapy efficacy and patient survival • STC1 interacts with CRT and traps CRT in mitochondria • STC1 impairs APC phagocytosis and T cell activation via trapping CRT • STC1 functions as an "eat-me" signal blocker and may be a phagocytosis checkpoint Lin et al. demonstrate tumor stanniocalcin-1 functions as an intracellular "eat-me" signal blocker by trapping calreticulin and impairs APC phagocytosis and T cell activation. Tumor stanniocalcin-1 negatively correlates with immunotherapy efficacy and patient survival. [ABSTRACT FROM AUTHOR]

Published
2021
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results