Your search keyword '"McCormick, Frank"' showing total 203 results

1. A Top-Down Proteomic Assay to Evaluate KRAS4B-Compound Engagement.

Author

D'Ippolito, Robert A., Rabara, Dana, Blanco, Maria Abreu, Alberico, Emily, Drew, Matthew R., Ramakrishnan, Nitya, Sontan, Dara, Widmeyer, Stephanie R. T., Scheidemantle, Grace M., Messing, Simon, Turner, David, Arkin, Michelle, Maciag, Anna E., Stephen, Andrew G., Esposito, Dominic, McCormick, Frank, Nissley, Dwight V., and DeHart, Caroline J.

Published

2024

2. A Top-Down Proteomic Assay to Evaluate KRAS4B-Compound Engagement

Author

D’Ippolito, Robert A., Rabara, Dana, Blanco, Maria Abreu, Alberico, Emily, Drew, Matthew R., Ramakrishnan, Nitya, Sontan, Dara, Widmeyer, Stephanie R. T., Scheidemantle, Grace M., Messing, Simon, Turner, David, Arkin, Michelle, Maciag, Anna E., Stephen, Andrew G., Esposito, Dominic, McCormick, Frank, Nissley, Dwight V., and DeHart, Caroline J.

Abstract

Development of new targeted inhibitors for oncogenic KRAS mutants may benefit from insight into how a given mutation influences the accessibility of protein residues and how compounds interact with mutant or wild-type KRAS proteins. Targeted proteomic analysis, a key validation step in the KRAS inhibitor development process, typically involves both intact mass- and peptide-based methods to confirm compound localization or quantify binding. However, these methods may not always provide a clear picture of the compound binding affinity for KRAS, how specific the compound is to the target KRAS residue, and how experimental conditions may impact these factors. To address this, we have developed a novel top-down proteomic assay to evaluate invitroKRAS4B-compound engagement while assessing relative quantitation in parallel. We present two applications to demonstrate the capabilities of our assay: maleimide-biotin labeling of a KRAS4BG12Dcysteine mutant panel and treatment of three KRAS4B proteins (WT, G12C, and G13C) with small molecule compounds. Our results show the time- or concentration-dependence of KRAS4B-compound engagement in context of the intact protein molecule while directly mapping the compound binding site.

Published

2024

3. Report From a Multidisciplinary Symposium on the Future of Living Kidney Donor Transplantation

Author

Peters, Thomas G., Fung, John J., Radcliffe-Richards, Janet, Satel, Sally, Roth, Alvin E., McCormick, Frank, Gershun, Martha, Matas, Arthur J., Roberts, John P., Morrison, Josh, Chertow, Glenn M., Lee, Laurie D., Held, Philip J., and Ojo, Akinlolu

Abstract

Virtually all clinicians agree that living donor renal transplantation is the optimal treatment for permanent loss of kidney function. Yet, living donor kidney transplantation has not grown in the United States for more than 2 decades. A virtual symposium gathered experts to examine this shortcoming and to stimulate and clarify issues salient to improving living donation. The ethical principles of rewarding kidney donors and the limits of altruism as the exclusive compelling stimulus for donation were emphasized. Concepts that donor incentives could save up to 40 000 lives annually and considerable taxpayer dollars were examined, and survey data confirmed voter support for donor compensation. Objections to rewarding donors were also presented. Living donor kidney exchanges and limited numbers of deceased donor kidneys were reviewed. Discussants found consensus that attempts to increase living donation should include removing artificial barriers in donor evaluation, expansion of living donor chains, affirming the safety of live kidney donation, and assurance that donors incur no expense. If the current legal and practice standards persist, living kidney donation will fail to achieve its true potential to save lives.

Published

2023

4. RAS Signaling Gone Awry in the Skin: The Complex Role of RAS in Cutaneous Neurofibroma Pathogenesis, Emerging Biological Insights

Author

Rhodes, Steven D., McCormick, Frank, Cagan, Ross L., Bakker, Annette, Staedtke, Verena, Ly, Ina, Steensma, Matthew R., Lee, Sang Y., Romo, Carlos G., Blakeley, Jaishri O., and Sarin, Kavita Y.

Abstract

Cutaneous neurofibromas (cNFs) are the most common tumor in people with the rasopathy neurofibromatosis type 1. They number in hundreds or even thousands throughout the body, and currently, there are no effective interventions to prevent or treat these skin tumors. To facilitate the identification of novel and effective therapies, essential studies including a more refined understanding of cNF biology and the role of RAS signaling and downstream effector pathways responsible for cNF initiation, growth, and maintenance are needed. This review highlights the current state of knowledge of RAS signaling in cNF pathogenesis and therapeutic development for cNF treatment.

Published

2023

5. A Call for Discovery and Therapeutic Development for Cutaneous Neurofibromas

Author

Blakeley, Jaishri O., Le, Lu Q., Lee, Sang Y., Ly, Ina, Rhodes, Steven D., Romo, Carlos G., Sarin, Kavita Y., Staedtke, Verena, Steensma, Matthew R., Wolkenstein, Pierre, Largaespada, David, Serra, Eduard, Haniffa, Muzlifah, Bakker, Annette, McCormick, Frank, Cagan, Ross L., Ju, William, Stemmer-Rachamimov, Anat, Grimes, Kevin, Topilko, Piotr, Kornacki, Deanna, Kelly, Kristen M., Gottesman, Sally, York, Zachary, and Epps, Roselyn

Published

2023

6. Beyond the basics: a perspective on barriers and opportunities for scaling up biochar production from forest slash

Author

Pierson, Derek, Anderson, Nathaniel, Brewen, Jessica, Clark, Nehalem, Hardy, Margaret C., McCollum, Daniel, McCormick, Frank H., Morisette, Jeffrey, Nicosia, Timothy, Page-Dumroese, Deborah, Rodriguez-Franco, Carlos, and Tirocke, Joanne

Abstract

Intertwined policy, economic, technology, and knowledge barriers underpin pervasive biochar adoption issues.Managers face pervasive challenges with permitting, slash handling costs and uncertain biochar application benefits.Pathways forward involve setting goals, streamlining permits, enhancing science communication, and further case studies.

Published

2024

7. Structure–function analysis of the SHOC2–MRAS–PP1C holophosphatase complex

Author

Kwon, Jason J., Hajian, Behnoush, Bian, Yuemin, Young, Lucy C., Amor, Alvaro J., Fuller, James R., Fraley, Cara V., Sykes, Abbey M., So, Jonathan, Pan, Joshua, Baker, Laura, Lee, Sun Joo, Wheeler, Douglas B., Mayhew, David L., Persky, Nicole S., Yang, Xiaoping, Root, David E., Barsotti, Anthony M., Stamford, Andrew W., Perry, Charles K., Burgin, Alex, McCormick, Frank, Lemke, Christopher T., Hahn, William C., and Aguirre, Andrew J.

Abstract

Receptor tyrosine kinase (RTK)–RAS signalling through the downstream mitogen-activated protein kinase (MAPK) cascade regulates cell proliferation and survival. The SHOC2–MRAS–PP1C holophosphatase complex functions as a key regulator of RTK–RAS signalling by removing an inhibitory phosphorylation event on the RAF family of proteins to potentiate MAPK signalling1. SHOC2 forms a ternary complex with MRAS and PP1C, and human germline gain-of-function mutations in this complex result in congenital RASopathy syndromes2–5. However, the structure and assembly of this complex are poorly understood. Here we use cryo-electron microscopy to resolve the structure of the SHOC2–MRAS–PP1C complex. We define the biophysical principles of holoenzyme interactions, elucidate the assembly order of the complex, and systematically interrogate the functional consequence of nearly all of the possible missense variants of SHOC2through deep mutational scanning. We show that SHOC2 binds PP1C and MRAS through the concave surface of the leucine-rich repeat region and further engages PP1C through the N-terminal disordered region that contains a cryptic RVXF motif. Complex formation is initially mediated by interactions between SHOC2 and PP1C and is stabilized by the binding of GTP-loaded MRAS. These observations explain how mutant versions of SHOC2 in RASopathies and cancer stabilize the interactions of complex members to enhance holophosphatase activity. Together, this integrative structure–function model comprehensively defines key binding interactions within the SHOC2–MRAS–PP1C holophosphatase complex and will inform therapeutic development .

Published

2022

8. Targeting CD70 in cutaneous T-cell lymphoma using an antibody-drug conjugate in patient-derived xenograft models

Author

Wu, Chi-Heng, Wang, Linlin, Yang, Chen-Yen, Wen, Kwun Wah, Hinds, Brian, Gill, Ryan, McCormick, Frank, Moasser, Mark, Pincus, Laura, and Ai, Weiyun Z.

Abstract

CD70 is a member of the tumor necrosis factor receptor superfamily. Emerging data indicate that CD70 may be a suitable target for various malignancies. We investigated the expression of CD70 in cutaneous and systemic T-cell lymphomas and conducted preclinical studies of SGN-CD70A, a CD70-directed antibody-drug conjugate (ADC), using patient-derived xenograft cutaneous T-cell lymphoma (CTCL PDX) models. CD70 expression was examined by immunohistochemical (IHC) stains in 49 diagnostic specimens of T-cell lymphomas. The activities of SGN-CD70A in growth inhibition and apoptosis induction were examined in CTCL cell lines and primary CTCL tumor cells. Using previously established CTCL PDXs, we conducted a dose-finding trial followed by a phase 2-like trial to evaluate the optimal dosing and the efficacy of SGN-CD70A in tumor-bearing PDX animals. The therapeutic efficacy of SGN-CD70A was measured by tumor-associated cell-free DNA (cfDNA) and survival of treated PDXs. We found that CD70 is highly expressed in T-cell lymphomas, especially in CTCL. SGN-CD70A inhibited cell growth and induced apoptosis in CD70-expressing CTCL cell lines and primary tumors cells. Additionally, SGN-CD70A at 100 μg/kg and 300 μg/kg prolonged the survival of PDXs in a dose-dependent manner. Finally, treatment with 3 doses of SGN-CD70A at 300 μg/kg was superior to a single-dose treatment in survival prolongation (median survival: 111 days vs 39 days; P = .017). Most importantly, multiple dosing of SGN-CD70A induced complete eradication of established tumors in PDXs measured by cfDNA. Our results demonstrated marked antitumor activity of SGN-CD70A in CTCL PDXs, providing compelling support for its clinical investigation.

Published

2022

9. Insights into the Cross Talk between Effector and Allosteric Lobes of KRAS from Methyl Conformational Dynamics

Author

Chao, Fa-An, Dharmaiah, Srisathiyanarayanan, Taylor, Troy, Messing, Simon, Gillette, William, Esposito, Dominic, Nissley, Dwight V., McCormick, Frank, Byrd, R. Andrew, Simanshu, Dhirendra K., and Cornilescu, Gabriel

Abstract

KRAS is the most frequently mutated RAS protein in cancer patients, and it is estimated that about 20% of the cancer patients in the United States carried mutant RAS proteins. To accelerate therapeutic development, structures and dynamics of RAS proteins had been extensively studied by various biophysical techniques for decades. Although 31P NMR studies revealed population equilibrium of the two major states in the active GMPPNP-bound form, more complex conformational dynamics in RAS proteins and oncogenic mutants subtly modulate the interactions with their downstream effectors. We established a set of customized NMR relaxation dispersion techniques to efficiently and systematically examine the ms-μs conformational dynamics of RAS proteins. This method allowed us to observe varying synchronized motions that connect the effector and allosteric lobes in KRAS. We demonstrated the role of conformational dynamics of KRAS in controlling its interaction with the Ras-binding domain of the downstream effector RAF1, the first kinase in the MAPK pathway. This allows one to explain, as well as to predict, the altered binding affinities of various KRAS mutants, which was neither previously reported nor apparent from the structural perspective.

Published

2022

10. Structure of the SHOC2–MRAS–PP1C complex provides insights into RAF activation and Noonan syndrome

Author

Bonsor, Daniel A., Alexander, Patrick, Snead, Kelly, Hartig, Nicole, Drew, Matthew, Messing, Simon, Finci, Lorenzo I., Nissley, Dwight V., McCormick, Frank, Esposito, Dominic, Rodriguez-Viciana, Pablo, Stephen, Andrew G., and Simanshu, Dhirendra K.

Abstract

SHOC2 acts as a strong synthetic lethal interactor with MEK inhibitors in multiple KRAS cancer cell lines. SHOC2 forms a heterotrimeric complex with MRAS and PP1C that is essential for regulating RAF and MAPK-pathway activation by dephosphorylating a specific phosphoserine on RAF kinases. Here we present the high-resolution crystal structure of the SHOC2–MRAS–PP1C (SMP) complex and apo-SHOC2. Our structures reveal that SHOC2, MRAS, and PP1C form a stable ternary complex in which all three proteins synergistically interact with each other. Our results show that dephosphorylation of RAF substrates by PP1C is enhanced upon interacting with SHOC2 and MRAS. The SMP complex forms only when MRAS is in an active state and is dependent on SHOC2 functioning as a scaffolding protein in the complex by bringing PP1C and MRAS together. Our results provide structural insights into the role of the SMP complex in RAF activation and how mutations found in Noonan syndrome enhance complex formation, and reveal new avenues for therapeutic interventions.

Published

2022

11. Cost Structures of US Organ Procurement Organizations

Author

Held, Philip J., Bragg-Gresham, Jennifer L., Peters, Thomas G., McCormick, Frank, Chertow, Glenn, Vaughan, William P., and Roberts, John P.

Abstract

Supplemental Digital Content is available in the text.

Published

2021

12. Sensitivity of Oncogenic KRAS-Expressing Cells to CDK9 Inhibition

Author

Lai, Lick Pui, Brel, Viviane, Sharma, Kanika, Frappier, Julia, Le-Henanf, Nadia, Vivet, Bertrand, Muzet, Nicolas, Schell, Emilie, Morales, Renaud, Rooney, Eamonn, Basse, Nicolas, Yi, Ming, Lacroix, Frederic, Holderfield, Matthew, Englaro, Walter, Marcireau, Christophe, Debussche, Laurent, Nissley, Dwight V., and McCormick, Frank

Abstract

Oncogenic forms of KRAS proteins are known to be drivers of pancreatic, colorectal, and lung cancers. The goal of this study is to identify chemical leads that inhibit oncogenic KRAS signaling. We first developed an isogenic panel of mouse embryonic fibroblast (MEF) cell lines that carry wild-type RAS, oncogenic KRAS, and oncogenic BRAF. We validated these cell lines by screening against a tool compound library of 1402 annotated inhibitors in an adenosine triphosphate (ATP)-based cell viability assay. Subsequently, this MEF panel was used to conduct a high-throughput phenotypic screen in a cell viability assay with a proprietary compound library. All 126 compounds that exhibited a selective activity against mutant KRAS were selected and prioritized based on their activities in secondary assays. Finally, five chemical clusters were chosen. They had specific activity against SW620 and LS513 over Colo320 colorectal cancer cell lines. In addition, they had no effects on BRAFV600E, MEK1, extracellular signal-regulated kinase 2 (ERK2), phosphoinositide 3-kinase alpha (PI3Kα), AKT1, or mammalian target of rapamycin (mTOR) as tested in in vitro enzymatic activity assays. Biophysical assays demonstrated that these compounds did not bind directly to KRAS. We further identified the mechanism of action and showed that three of them have CDK9 inhibitory activity. In conclusion, we have developed and validated an isogenic MEF panel that was used successfully to identify RAS oncogenic or wild-type allele-specific vulnerabilities. Furthermore, we identified sensitivity of oncogenic KRAS-expressing cells to CDK9 inhibitors, which warrants future studies of treating KRAS-driven cancers with CDK9 inhibitors.

Published

2021

13. Sensitivity of Oncogenic KRAS-Expressing Cells to CDK9 Inhibition

Author

Lai, Lick Pui, Brel, Viviane, Sharma, Kanika, Frappier, Julia, Le-Henanf, Nadia, Vivet, Bertrand, Muzet, Nicolas, Schell, Emilie, Morales, Renaud, Rooney, Eamonn, Basse, Nicolas, Yi, Ming, Lacroix, Frederic, Holderfield, Matthew, Englaro, Walter, Marcireau, Christophe, Debussche, Laurent, Nissley, Dwight V., and McCormick, Frank

Abstract

Oncogenic forms of KRAS proteins are known to be drivers of pancreatic, colorectal, and lung cancers. The goal of this study is to identify chemical leads that inhibit oncogenic KRAS signaling. We first developed an isogenic panel of mouse embryonic fibroblast (MEF) cell lines that carry wild-type RAS, oncogenic KRAS, and oncogenic BRAF. We validated these cell lines by screening against a tool compound library of 1402 annotated inhibitors in an adenosine triphosphate (ATP)-based cell viability assay. Subsequently, this MEF panel was used to conduct a high-throughput phenotypic screen in a cell viability assay with a proprietary compound library. All 126 compounds that exhibited a selective activity against mutant KRAS were selected and prioritized based on their activities in secondary assays. Finally, five chemical clusters were chosen. They had specific activity against SW620 and LS513 over Colo320 colorectal cancer cell lines. In addition, they had no effects on BRAFV600E, MEK1, extracellular signal-regulated kinase 2 (ERK2), phosphoinositide 3-kinase alpha (PI3Kα), AKT1, or mammalian target of rapamycin (mTOR) as tested in in vitro enzymatic activity assays. Biophysical assays demonstrated that these compounds did not bind directly to KRAS. We further identified the mechanism of action and showed that three of them have CDK9 inhibitory activity. In conclusion, we have developed and validated an isogenic MEF panel that was used successfully to identify RAS oncogenic or wild-type allele-specific vulnerabilities. Furthermore, we identified sensitivity of oncogenic KRAS-expressing cells to CDK9 inhibitors, which warrants future studies of treating KRAS-driven cancers with CDK9 inhibitors.

Published

2021

14. Reducing the Shortage of Transplant Kidneys: A Lost Opportunity for the US Health Resources and Services Administration (HRSA)

Author

McCormick, Frank, Held, Philip J., Chertow, Glenn M., Peters, Thomas G., and Roberts, John P.

Published

2021

15. Cutaneous T-Cell Lymphoma PDX Drug Screening Platform Identifies Cooperation between Inhibitions of PI3Kα/δ and HDAC

Author

Wu, Chi-Heng, Yang, Chen-Yen, Wang, Linlin, Gao, Hua-Xin, Rakhshandehroo, Taha, Afghani, Shervin, Pincus, Laura, Balassanian, Ronald, Rubenstein, James, Gill, Ryan, Bandyopadhyay, Sourav, McCormick, Frank, Moasser, Mark, and Ai, Weiyun Z.

Abstract

Cutaneous T-cell lymphoma is a form of non-Hodgkin lymphoma that manifests initially in the skin and disseminates systemically as the disease progresses. Mycosis fungoides and Sézary syndrome are the most common subtypes of cutaneous T-cell lymphoma. Advanced mycosis fungoides and Sézary syndrome are life threatening with few treatment options. We searched for new agents by high-throughput screening of selected targeted compounds and identified high-value targets, including phosphatidylinositol 3-kinase (PI3K) and cyclin-dependent kinases. To validate these hits from the screen, we developed patient-derived xenograft mouse models that recapitulated the cardinal features of mycosis fungoides and Sézary syndrome and maintained histologic and molecular characteristics of their clinical counterparts. Importantly, we established a blood-based biomarker assay using tumor cell-free DNA to measure systemic tumor burden longitudinally in living mice during drug therapy. A PI3K inhibitor, BKM120, was tested in our patient-derived xenograft model leading to disease attenuation and prolonged survival. Isoform-specific small interfering RNA knockdowns and isoform-selective PI3K inhibitors identified PI3K-δ as required for tumor proliferation. Additional studies showed a synergistic combination of PI3K-α/δ inhibitors with histone deacetylase inhibitors. The strong preclinical efficacy of this potent combination against multiple patient-derived xenograft models makes it an excellent candidate for further clinical development.

Published

2021

16. Evidence-Based Physical Examination for the Diagnosis of Subscapularis Tears: A Systematic Review

Author

Dakkak, Andrew, Krill, Michael K., Krill, Matthew L., Nwachukwu, Benedict, and McCormick, Frank

Abstract

Context: There is a renewed interest in diagnosing and treating subscapularis tears, but there is a paucity of clinical guidance to optimize diagnostic decision-making.Objective: To perform a literature review to evaluate advanced maneuvers and special tests in the diagnosis of subscapularis tears and create a diagnostic algorithm for subscapularis pathology.Data Sources: PubMed, MEDLINE, Ovid, and Cochrane Reviews databases.Study Selection: Inclusion criteria consisted of level 1 and 2 studies published in peer-reviewed scientific journals that focused on physical examination.Study Design: Systematic review.Level of Evidence: Level 2.Data Extraction: Individual test characteristics (bear hug, belly press, lift-off, Napoleon, and internal rotation lag sign) were combined in series and in parallel to maximize clinical sensitivity and specificity for any special test evaluated in at least 2 studies. A secondary analysis utilized subjective pretest probabilities to create a clinical decision tree algorithm and provide posttest probabilities.Results: A total of 3174 studies were identified, and 5 studies met inclusion criteria. The special test combination of the bear hug and belly press demonstrated the highest positive likelihood ratio (18.29). Overall, 3 special test combinations in series demonstrated a significant impact on posttest probabilities. With parallel testing, the combination of bear hug and belly press had the highest sensitivity (84%) and lowest calculated negative likelihood ratio (0.21).Conclusion: The combined application of the bear hug and belly press physical examination maneuvers is an optimal combination for evaluating subscapularis pathology. Positive findings using this test combination in series with a likely pretest probability yield a 96% posttest probability; whereas, negative findings tested in parallel with an unlikely pretest probability yield a 12% posttest probability.

Published

2021

17. Minor intron retention drives clonal hematopoietic disorders and diverse cancer predisposition

Author

Inoue, Daichi, Polaski, Jacob T., Taylor, Justin, Castel, Pau, Chen, Sisi, Kobayashi, Susumu, Hogg, Simon J., Hayashi, Yasutaka, Pineda, Jose Mario Bello, El Marabti, Ettaib, Erickson, Caroline, Knorr, Katherine, Fukumoto, Miki, Yamazaki, Hiromi, Tanaka, Atsushi, Fukui, Chie, Lu, Sydney X., Durham, Benjamin H., Liu, Bo, Wang, Eric, Mehta, Sanjoy, Zakheim, Daniel, Garippa, Ralph, Penson, Alex, Chew, Guo-Liang, McCormick, Frank, Bradley, Robert K., and Abdel-Wahab, Omar

Abstract

Most eukaryotes harbor two distinct pre-mRNA splicing machineries: the major spliceosome, which removes >99% of introns, and the minor spliceosome, which removes rare, evolutionarily conserved introns. Although hypothesized to serve important regulatory functions, physiologic roles of the minor spliceosome are not well understood. For example, the minor spliceosome component ZRSR2 is subject to recurrent, leukemia-associated mutations, yet functional connections among minor introns, hematopoiesis and cancers are unclear. Here, we identify that impaired minor intron excision via ZRSR2 loss enhances hematopoietic stem cell self-renewal. CRISPR screens mimicking nonsense-mediated decay of minor intron-containing mRNA species converged on LZTR1, a regulator of RAS-related GTPases. LZTR1minor intron retention was also discovered in the RASopathy Noonan syndrome, due to intronic mutations disrupting splicing and diverse solid tumors. These data uncover minor intron recognition as a regulator of hematopoiesis, noncoding mutations within minor introns as potential cancer drivers and links among ZRSR2mutations, LZTR1 regulation and leukemias.

Published

2021

18. RAS-targeted therapies: is the undruggable drugged?

Author

Moore, Amanda R., Rosenberg, Scott C., McCormick, Frank, and Malek, Shiva

Abstract

RAS(KRAS, NRASand HRAS) is the most frequently mutated gene family in cancers, and, consequently, investigators have sought an effective RAS inhibitor for more than three decades. Even 10 years ago, RAS inhibitors were so elusive that RAS was termed ‘undruggable’. Now, with the success of allele-specific covalent inhibitors against the most frequently mutated version of RAS in non-small-cell lung cancer, KRASG12C, we have the opportunity to evaluate the best therapeutic strategies to treat RAS-driven cancers. Mutation-specific biochemical properties, as well as the tissue of origin, are likely to affect the effectiveness of such treatments. Currently, direct inhibition of mutant RAS through allele-specific inhibitors provides the best therapeutic approach. Therapies that target RAS-activating pathways or RAS effector pathways could be combined with these direct RAS inhibitors, immune checkpoint inhibitors or T cell-targeting approaches to treat RAS-mutant tumours. Here we review recent advances in therapies that target mutant RAS proteins and discuss the future challenges of these therapies, including combination strategies.

Published

2020

19. The duality of human oncoproteins: drivers of cancer and congenital disorders

Author

Castel, Pau, Rauen, Katherine A., and McCormick, Frank

Abstract

Human oncoproteins promote transformation of cells into tumours by dysregulating the signalling pathways that are involved in cell growth, proliferation and death. Although oncoproteins were discovered many years ago and have been widely studied in the context of cancer, the recent use of high-throughput sequencing techniques has led to the identification of cancer-associated mutations in other conditions, including many congenital disorders. These syndromes offer an opportunity to study oncoprotein signalling and its biology in the absence of additional driver or passenger mutations, as a result of their monogenic nature. Moreover, their expression in multiple tissue lineages provides insight into the biology of the proto-oncoprotein at the physiological level, in both transformed and unaffected tissues. Given the recent paradigm shift in regard to how oncoproteins promote transformation, we review the fundamentals of genetics, signalling and pathogenesis underlying oncoprotein duality.

Published

2020

20. The cost of procuring deceased donor kidneys: Evidence from OPO cost reports 2013‐2017

Author

Held, Philip J., Bragg‐Gresham, Jennifer L., Peters, Thomas, Chertow, Glen M., McCormick, Frank, and Roberts, John P.

Abstract

Using 5 years of US organ procurement organization (OPO) data, we determined the cost of recovering a viable (ie, transplanted) kidney for each of 51 OPOs. We also examined the effects on OPO costs of the recovery of nonviable (ie, discarded) kidneys and other OPO metrics. Annual cost reports from 51 independent OPOs were used to determine the cost per recovered kidney for each OPO. A quadratic regression model was employed to estimate the relationship between the cost of kidneys and the number of viable kidneys recovered, as well as other OPO performance indicators. The cost of transplanted kidneys at individual OPOs ranged widely from $24 000 to $56 000, and the average was $36 000. The cost of a viable kidney tended to decline with the number of kidneys procured up to 549 kidneys per year and then increase. Of the total 81 401 kidneys recovered, 66 454 were viable and 14 947 (18.4%) were nonviable. The costs of kidneys varied widely over the OPOs studied, and costs were a function of the recovered number of viable and nonviable organs, local cost levels, donation after cardiac death, year, and Standardized Donor Rate Ratio. Cost increases were 3% per year. The costs of deceased donor kidneys vary widely over the organ procurement organizations studied, and costs are a function of the recovered number of viable and nonviable organs, local cost levels, donation after cardiac death, year, and standardized donor rate ratio.

Published

2020

21. Outcomes of Primary Biceps Subpectoral Tenodesis in an Active Population: A Prospective Evaluation of 101 Patients.

Author

Provencher, Matthew T., McCormick, Frank, Peebles, Liam A., Beaulieu-Jones, Brendin R., Dekker, Travis J., LeClere, Lance E., Anthony, Shawn, Solomon, Daniel J., Golijanin, Petar, and Dewing, Christopher

Abstract

Purpose: To evaluate the surgical outcomes of a primary subpectoral biceps tenodesis for long head of the biceps tendon (LHBT) pathology in a large cohort of prospectively, serially collected, patients in a young active population that has known high physical demands and requirements of their shoulder to perform their vocation.Methods: A retrospective review of prospectively collected data from an active military personnel with a diagnosis of a Type II SLAP tear or biceps tenosynovitis was performed. Outcomes were evaluated at a minimum follow-up time of 18 months based on preoperative and postoperative assessments of the Single Assessment Numeric Evaluation, Western Ontario Rotator Cuff index, biceps position, and return to active duty. Inclusion criteria were (1) SLAP tears on magnetic resonance arthrogram (classified into SLAP group), and (2) no SLAP tear but examination findings of biceps tendonitis (placed in the LHBT tendonitis group). Patients were excluded for full-thickness rotator cuff tears, high-grade partial thickness tears requiring repair, acromioclavicular joint pathology, and labral pathology outside of the SLAP lesion. Patients from both groups subsequently were treated with open, subpectoral tenodesis.Results: Over a 6-year period at a mean follow-up of 2.75 years (range 1.5-5.7 years), 125 active-duty military personnel with mean age of 42.6 years (range 26.3-56.5) were enrolled. A total of 101 of 125 patients (81%) completed study requirements at a mean of 2.75 years (range 1.5-5.7 years). In total, 40 patients were diagnosed with type II SLAP tears (39.6%) and 61 with biceps tendonitis without SLAP tear (60.4%). Following open, subpectoral tenodesis, there was a significant improvement in patient outcomes (Western Ontario Rotator Cuff = 54% preoperative vs 89% postoperative, Single Assessment Numeric Evaluation = 58 preoperative vs 89.5 postoperative, P < .01). In total, 82% of patients returned to full activity at a mean of 4.1 months. The biceps muscle measured relative to the antecubital fossa of operative (mean 3.20 cm) versus nonoperative (3.11 cm) was not clinically different (P = .57). There was an 8% complication rate, including 3 requiring revision, 2 superficial infections, and 3 transient neurapraxias.Conclusions: Primary subpectoral open biceps tenodesis for SLAP tears or pathology of the LHBT provides significant improvement in shoulder outcomes with a reliable return to activity level with low risk for complications.Level Of Evidence: Level IV (Case series). [ABSTRACT FROM AUTHOR]

Published

2019

22. A concise evidence-based physical examination for diagnosis of acromioclavicular joint pathology: a systematic review.

Author

Krill, Michael K., Rosas, Samuel, Kwon, Kihyun, Dakkak, Andrew, Nwachukwu, Benedict U., and Mccormick, Frank

Abstract

Objectives: The clinical examination of the shoulder joint is an undervalued diagnostic tool for evaluating acromioclavicular (AC) joint pathology. Applying evidence-based clinical tests enables providers to make an accurate diagnosis and minimize costly imaging procedures and potential delays in care. The purpose of this study was to create a decision tree analysis enabling simple and accurate diagnosis of AC joint pathology. Methods: A systematic review of the Medline, Ovid and Cochrane Review databases was performed to identify level one and two diagnostic studies evaluating clinical tests for AC joint pathology. Individual test characteristics were combined in series and in parallel to improve sensitivities and specificities. A secondary analysis utilized subjective pre-test probabilities to create a clinical decision tree algorithm with post-test probabilities. Results: The optimal special test combination to screen and confirm AC joint pathology combined Paxinos sign and O’Brien’s Test, with a specificity of 95.8% when performed in series; whereas, Paxinos sign and Hawkins-Kennedy Test demonstrated a sensitivity of 93.7% when performed in parallel. Paxinos sign and O’Brien’s Test demonstrated the greatest positive likelihood ratio (2.71); whereas, Paxinos sign and Hawkins-Kennedy Test reported the lowest negative likelihood ratio (0.35). Conclusion: No combination of special tests performed in series or in parallel creates more than a small impact on post-test probabilities to screen or confirm AC joint pathology. Paxinos sign and O’Brien’s Test is the only special test combination that has a small and sometimes important impact when used both in series and in parallel. Physical examination testing is not beneficial for diagnosis of AC joint pathology when pretest probability is unequivocal. In these instances, it is of benefit to proceed with procedural tests to evaluate AC joint pathology. Ultrasound-guided corticosteroid injections are diagnostic and therapeutic. An ultrasound-guided AC joint corticosteroid injection may be an appropriate new standard for treatment and surgical decision-making. Level of Evidence: II – Systematic Review. [ABSTRACT FROM PUBLISHER]

Published

2018

23. SPRED proteins and their roles in signal transduction, development, and malignancy

Author

Lorenzo, Claire and McCormick, Frank

Abstract

In this review, Lorenzo and McCormick summarize and discuss biochemical, structural, and biological functions of SPRED proteins, including their roles in normal cell growth, differentiation, and human disease.

Published

2020

24. Feasibility of using NF1-GRD and AAV for gene replacement therapy in NF1-associated tumors

Author

Bai, Ren-Yuan, Esposito, Dominic, Tam, Ada, McCormick, Frank, Riggins, Gregory, Wade Clapp, D., and Staedtke, Verena

Abstract

Neurofibromatosis type 1, including the highly aggressive malignant peripheral nerve sheath tumors (MPNSTs), is featured by the loss of functional neurofibromin 1 (NF1) protein resulting from genetic alterations. A major function of NF1 is suppressing Ras activities, which is conveyed by an intrinsic GTPase-activating protein-related domain (GRD). In this study, we explored the feasibility of restoring Ras GTPase via exogenous expression of various GRD constructs, via gene delivery using a panel of adeno-associated virus (AAV) vectors in MPNST and human Schwann cells (HSCs). We demonstrated that several AAV serotypes achieved favorable transduction efficacies in those cells and a membrane-targeting GRD fused with an H-Ras C-terminal motif (C10) dramatically inhibited the Ras pathway and MPNST cells in a NF1-specific manner. Our results opened up a venue of gene replacement therapy in NF1-related tumors.

Published

2019

25. KRAS Prenylation Is Required for Bivalent Binding with Calmodulin in a Nucleotide-Independent Manner

Author

Agamasu, Constance, Ghirlando, Rodolfo, Taylor, Troy, Messing, Simon, Tran, Timothy H., Bindu, Lakshman, Tonelli, Marco, Nissley, Dwight V., McCormick, Frank, and Stephen, Andrew G.

Abstract

Deregulation of KRAS4b signaling pathway has been implicated in 30% of all cancers. Membrane localization of KRAS4b is an essential step for the initiation of the downstream signaling cascades that guide various cellular mechanisms. KRAS4b plasma membrane (PM) binding is mediated by the insertion of a prenylated moiety that is attached to the terminal carboxy-methylated cysteine, in addition to electrostatic interactions of its positively charged hypervariable region with anionic lipids. Calmodulin (CaM) has been suggested to selectively bind KRAS4b to act as a negative regulator of the RAS/mitogen-activated protein kinase (MAPK) signaling pathway by displacing KRAS4b from the membrane. However, the mechanism by which CaM can recognize and displace KRAS4b from the membrane is not well understood. In this study, we employed biophysical and structural techniques to characterize this mechanism in detail. We show that KRAS4b prenylation is required for binding to CaM and that the hydrophobic pockets of CaM can accommodate the prenylated region of KRAS4b, which might represent a novel CaM-binding motif. Remarkably, prenylated KRAS4b forms a 2:1 stoichiometric complex with CaM in a nucleotide-independent manner. The interaction between prenylated KRAS4b and CaM is enthalpically driven, and electrostatic interactions also contribute to the formation of the complex. The prenylated KRAS4b terminal KSKTKC-farnesylation and carboxy-methylation is sufficient for binding and defines the minimal CaM-binding motif. This is the same region implicated in membrane and phosphodiesterase6-δbinding. Finally, we provide a structure-based docking model by which CaM binds to prenylated KRAS4b. Our data provide new insights into the KRAS4b-CaM interaction and suggest a possible mechanism whereby CaM can regulate KRAS4b membrane localization.

Published

2019

26. RAS-targeted therapies

Author

Moore, Amanda R., Rosenberg, Scott C., McCormick, Frank, and Malek, Shiva

Abstract

Therapies targeting RAS, a small GTPase that is frequently altered in cancer, are explored in this poster.

Published

2024

27. Trends in sports-related concussion diagnoses in the USA: a population-based analysis using a private-payor database.

Author

Achampong, Kelms Amoo, Rosas, Samuel, Schmoke, Nicholas, Accilien, Yves-Dany, Nwachukwu, Benedict U., and McCormick, Frank

Abstract

Objective: To describe recent epidemiological trends in concussion diagnosis within the United States (US) population. Methods: We conducted a retrospective review of PearlDiver, a private-payor insurance database. Our search included International Classification of Disease, Ninth Revision codes for sports-related concussions spanning 2010 through 2014. Overall study population included patients aged 5 to 39 with subgroup analysis performed on Cohort A (Youth), children and adolescents aged 5 to 19, and Cohort B (Adults), adults aged 20 to 39. Incidence was defined as the number of individuals diagnosed normalized to the number of patients in the database for each demographic. Results: Our search returned 1,599 patients diagnosed during the study period. The average (±SD) annual rate was 4.14 ± 1.42 per 100,000 patients for the overall population. Youth patients were diagnosed at a mean annual rate of 3.78 ± 1.30 versus 0.36 ± 0.16 per 100,000 in Adults. Concussion normalized incidence significantly increased from 2.47 to 3.87 per 100,000 patients (57%) in the Youth cohort (p = 0.048). In Adults, rate grew from 0.34 to 0.44 per 100,000 patients (29%) but was not statistically significant (p = 0.077). Four-year compound annual growth rates for Youth and Adults were 26.3% and 20.4%, respectively. Youth patients comprised 1,422/1,599 (90.18%) of all concussion diagnoses and were predominantly male (75%). Adults also constituted 138/1,599 (8.63%) of the sample and were also largely male (80%). Midwestern states had highest diagnostic rates (Cohort A:19 per 100,000 and Cohort B:1.8 per 100,000). Both cohorts had the most total diagnoses made in the fourth quarter followed by the second quarter. Conclusion: Sports-related concussion diagnostic rates have grown significantly in the youth population. Quarterly, regional and gender distributions appear consistent with participation in concussion- prone sports. Utilization of individualized and multifaceted approaches are recommended to advance diagnosis, assessment and management of concussions in the U.S. population. [ABSTRACT FROM AUTHOR]

Published

2017

28. A practical, evidence-based, comprehensive (PEC) physical examination for diagnosing pathology of the long head of the biceps.

Author

Rosas, Samuel, Krill, Michael K., Amoo-Achampong, Kelms, Kwon, KiHyun, Nwachukwu, Benedict U., and McCormick, Frank

Abstract

Background Clinical examination of the shoulder joint has gained attention as clinicians aim to use an evidence-based examination of the biceps tendon, with the desire for a proper diagnosis while minimizing costly imaging procedures. The purpose of this study is to create a decision tree analysis that enables the development of a clinical algorithm for diagnosing long head of biceps (LHB) pathology. Methods A literature review of Level I and II diagnostic studies was conducted to extract characteristics of clinical tests for LHB pathology through a systematic review of PubMed, Medline, Ovid, and Cochrane Review databases. Tests were combined in series and parallel to determine sensitivities and specificities, and positive and negative likelihood ratios were determined for each combination using a subjective pretest probability. The “gold standard” for diagnosis in all included studies was arthroscopy or arthrotomy. Results The optimal testing modality was use of the uppercut test combined with the tenderness to palpation of the biceps tendon test. This combination achieved a sensitivity of 88.4% when performed in parallel and a specificity of 93.8% when performed in series. These tests used in combination optimize post-test probability accuracy greater than any single individual test. Conclusion Performing the uppercut test and biceps groove tenderness to palpation test together has the highest sensitivity and specificity of known physical examinations maneuvers to aid in the diagnosis of LHB pathology compared with diagnostic arthroscopy (practical, evidence-based, comprehensive examination). A decision tree analysis aides in the practical, evidence-based, comprehensive examination diagnostic accuracy post-testing based on the ordinal scale pretest probability. [ABSTRACT FROM AUTHOR]

Published

2017

29. Aurora kinase A drives the evolution of resistance to third-generation EGFR inhibitors in lung cancer

Author

Shah, Khyati N., Bhatt, Roma, Rotow, Julia, Rohrberg, Julia, Olivas, Victor, Wang, Victoria E., Hemmati, Golzar, Martins, Maria M., Maynard, Ashley, Kuhn, Jonathan, Galeas, Jacqueline, Donnella, Hayley J., Kaushik, Swati, Ku, Angel, Dumont, Sophie, Krings, Gregor, Haringsma, Henry J., Robillard, Liliane, Simmons, Andrew D., Harding, Thomas C., McCormick, Frank, Goga, Andrei, Blakely, Collin M., Bivona, Trever G., and Bandyopadhyay, Sourav

Abstract

Although targeted therapies often elicit profound initial patient responses, these effects are transient due to residual disease leading to acquired resistance. How tumors transition between drug responsiveness, tolerance and resistance, especially in the absence of preexisting subclones, remains unclear. In epidermal growth factor receptor (EGFR)-mutant lung adenocarcinoma cells, we demonstrate that residual disease and acquired resistance in response to EGFR inhibitors requires Aurora kinase A (AURKA) activity. Nongenetic resistance through the activation of AURKA by its coactivator TPX2 emerges in response to chronic EGFR inhibition where it mitigates drug-induced apoptosis. Aurora kinase inhibitors suppress this adaptive survival program, increasing the magnitude and duration of EGFR inhibitor response in preclinical models. Treatment-induced activation of AURKA is associated with resistance to EGFR inhibitors in vitro, in vivo and in most individuals with EGFR-mutant lung adenocarcinoma. These findings delineate a molecular path whereby drug resistance emerges from drug-tolerant cells and unveils a synthetic lethal strategy for enhancing responses to EGFR inhibitors by suppressing AURKA-driven residual disease and acquired resistance.

Published

2019

30. Historical Perspectives and a New U.S. Forest Service Strategy for Fish and Aquatic Stewardship

Author

Shively, Dan, Rothlisberger, John D., Gillespie, Nathaniel, Dombeck, Mike, Moore, Virgil, Roghair, Craig, Demario, Devin, McCormick, Frank, and Weldon, Leslie

Abstract

The U.S. Forest Service has a long, rich history of helping to steward the nation's fish and aquatic resources and contributing to the broader fish and aquatic conservation and scientific community in the United States and worldwide. The agency recently updated its national strategy for fish and aquatic resource stewardship. The new strategy builds on 30 years of lessons learned through implementing the agency's original Rise to the Future: National Fish and Aquatic Strategy, the first national freshwater fisheries strategy by a federal agency. It also addresses 21st century challenges, establishing a stronger foundation for integrated aquatic resource stewardship throughout the agency and renewing an emphasis on cooperation with local, state, federal, and tribal governments and partnering with nongovernmental organizations, private landowners and water users, private businesses, the sportfishing industry, and others. The new strategy outlines six goals that provide a robust framework to guide future efforts: (1) conserve fish and aquatic resources; (2) connect people to the outdoors through fishing, boating, and other aquatic activities; (3) strengthen partnerships and work across boundaries; (4) deliver and apply scientific research; (5) build capacity through mentoring and training; and (6) communicate the value of fish and aquatic resources.

Published

2018

31. Differential Effector Engagement by Oncogenic KRAS

Author

Yuan, Tina L., Amzallag, Arnaud, Bagni, Rachel, Yi, Ming, Afghani, Shervin, Burgan, William, Fer, Nicole, Strathern, Leslie A., Powell, Katie, Smith, Brian, Waters, Andrew M., Drubin, David, Thomson, Ty, Liao, Rosy, Greninger, Patricia, Stein, Giovanna T., Murchie, Ellen, Cortez, Eliane, Egan, Regina K., Procter, Lauren, Bess, Matthew, Cheng, Kwong Tai, Lee, Chih-Shia, Lee, Liam Changwoo, Fellmann, Christof, Stephens, Robert, Luo, Ji, Lowe, Scott W., Benes, Cyril H., and McCormick, Frank

Abstract

KRAS can bind numerous effector proteins, which activate different downstream signaling events. The best known are RAF, phosphatidylinositide (PI)-3′ kinase, and RalGDS families, but many additional direct and indirect effectors have been reported. We have assessed how these effectors contribute to several major phenotypes in a quantitative way, using an arrayed combinatorial siRNA screen in which we knocked down 41 KRAS effectors nodes in 92 cell lines. We show that every cell line has a unique combination of effector dependencies, but in spite of this heterogeneity, we were able to identify two major subtypes of KRAS mutant cancers of the lung, pancreas, and large intestine, which reflect different KRAS effector engagement and opportunities for therapeutic intervention.

Published

2018

32. An orthopedist’s guide to shoulder ultrasound: a systematic review of examination protocols.

Author

Amoo-Achampong, Kelms, Nwachukwu, Benedict U., and McCormick, Frank

Abstract

Background: The utilization of musculoskeletal ultrasound has expanded within the setting of the orthopedic clinic as a cost-effective, point-of-care diagnostic tool for shoulder pathology. In experienced hands, ultrasound exhibits capabilities equivalent to that of magnetic resonance imaging in the diagnosis of many shoulder diseases including full-thickness and partial-thickness rotator cuff tears. Although similarly effective in identifying additional shoulder disease processes, major obstacles to its widespread use include user dependence and intrinsic limitation to extra-articular diagnosis. Objectives: The purpose of this review is to present a step-by-step guide of how to perform a comprehensive shoulder examination and to discuss the appropriate use, economic benefit and implementation of ultrasound within the clinic. Methods: A systematic search (June 2016) of PubMed, Scopus, and EMBASE databases was conducted according to the Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) guidelines for literature presenting shoulder ultrasound examination protocols. Included studies were peer-reviewed articles or academic society endorsed protocols presenting comprehensive sonographic examinations of the adult shoulder. Papers with limited or single structure examination descriptions, non-English language, and publication dates before 1980 were excluded. Final papers meeting criteria were secondarily screened for publication after 2005 to reflect the current state of ultrasound imaging. Results and Conclusions: The search yielded 1,725 unique articles with 17 studies meeting final selection criteria. Information from identified studies was summarized to formulate a 4-part shoulder examination protocol, including steps most pertinent to orthopedic in-office diagnoses. In agreement with previous studies, the inexperienced orthopedic surgeon can be quickly trained to expert level proficiency in shoulder ultrasound diagnosis. Using an established protocol, a comprehensive, yet effective shoulder ultrasound examination can be performed within ten minutes. Further, ultrasound provides opportunity to off-set costs through the engagement of revenue generating activity for the orthopedic practice. [ABSTRACT FROM AUTHOR]

Published

2016

33. Patient Satisfaction Reporting for the Treatment of Femoroacetabular Impingement.

Author

Kahlenberg, Cynthia A., Nwachukwu, Benedict U., Schairer, William W., McCormick, Frank, and Ranawat, Anil S.

Abstract

Purpose: The purpose of this study was to evaluate how patient satisfaction after surgical femoroacetabular impingement (FAI) treatment is measured and reported in the current evidence base.Methods: A review of the MEDLINE database was performed. Clinical outcome studies of FAI that reported a measure of patient satisfaction were included. Patient demographics, clinical outcome scores, and patient satisfaction measures were extracted. The NewCastle Ottawa Scale (NOS) was used to grade quality. Statistical analysis was primarily descriptive.Results: Twenty-six studies met inclusion criteria; the mean NOS score among included studies was 5.7. Most studies were level 3 or 4 (n = 25, 96.1%). A 0 to 10 numeric scale, described by some studies as a visual analog scale, was the most commonly used method to assess satisfaction (n = 21; 80.8%), and mean reported scores ranged from 6.8 to 9.2 out of 10. Four studies (15.4%) used an ordinal scale, and 1 study (3.8%) used willingness to undergo surgery again as the measure of satisfaction. None of the included studies assessed preoperative satisfaction or patient expectation. Pooled cohort analysis was limited by significant overlapping study populations. Predictors of patients' satisfaction identified in included studies were presence of arthritis and postoperative outcome scores.Conclusions: Patient satisfaction was not uniformly assessed in the literature. Most studies used a 0- to 10-point satisfaction scale, but none distinguished between the process of care and the outcome of care. Although satisfaction scores were generally high, the quality of the methodologies in the studies that reported satisfaction was low, and the studies likely included overlapping patient populations. More work needs to be done to develop standardized ways for assessing patient satisfaction after arthroscopic hip surgery and other procedures in orthopaedic sports medicine.Level Of Evidence: Level III, systematic review of Level III studies. [ABSTRACT FROM AUTHOR]

Published

2016

34. Arthroplasty for the surgical management of complex proximal humerus fractures in the elderly: a cost-utility analysis.

Author

Nwachukwu, Benedict U., Schairer, William W., McCormick, Frank, Dines, David M., Craig, Edward V., and Gulotta, Lawrence V.

Abstract

Background Shoulder hemiarthroplasty (HA) has been the standard treatment for complex proximal humerus fractures in the elderly requiring surgery but not amenable to fixation. Reverse total shoulder arthroplasty (RTSA) has also emerged as a costly albeit highly effective alternative. The purpose of this study was to compare the cost-effectiveness of nonoperative fracture care, HA, and RTSA for complex proximal humerus fractures from the perspective of both U.S. payors and hospitals. Methods A Markov model was constructed for the treatment alternatives. Costs were expressed in 2013 U.S. dollars and effectiveness in quality-adjusted life-years (QALYs). The principal outcome measure was incremental cost-effectiveness ratio (ICER). Sensitivity analyses were performed to evaluate model assumptions. Results In the base case, from the payor perspective, RTSA was associated with an ICER of $8100/QALY; HA was eliminated from payor analysis as a cost-ineffective strategy. From the hospital perspective, however, HA was not cost-ineffective and the ICER for HA was $36,700/QALY, with RTSA providing incremental effectiveness at $57,400/QALY. RTSA was the optimal strategy in 61% and 54% of payor and hospital probabilistic sensitivity analyses, respectively. The preferred strategy was dependent on associated QALY gains, primary RTSA cost, and failure rates for RTSA. Conclusions RTSA can be a cost-effective intervention in the surgical treatment of complex proximal humerus fractures. HA can also be a cost-effective intervention, depending on the cost perspective (cost-ineffective for payor but cost-effective for the hospital). This analysis highlights the opportunities for increased cost-sharing strategies to alleviate the cost burden on hospitals. [ABSTRACT FROM AUTHOR]

Published

2016

35. Use of Hip Arthroscopy and Risk of Conversion to Total Hip Arthroplasty: A Population-Based Analysis.

Author

Schairer, William W., Nwachukwu, Benedict U., McCormick, Frank, Lyman, Stephen, and Mayman, David

Abstract

Purpose: To use population-level data to (1) evaluate the conversion rate of total hip arthroplasty (THA) within 2 years of hip arthroscopy and (2) assess the influence of age, arthritis, and obesity on the rate of conversion to THA.Methods: We used the State Ambulatory Surgery Databases and State Inpatient Databases for California and Florida from 2005 through 2012, which contain 100% of patient visits. Hip arthroscopy patients were tracked for subsequent primary THA within 2 years. Out-of-state patients and patients with less than 2 years follow-up were excluded. Multivariate analysis identified risks for subsequent hip arthroplasty after arthroscopy.Results: We identified 7,351 patients who underwent hip arthroscopy with 2 years follow-up. The mean age was 43.9 ± 13.7 years, and 58.8% were female patients. Overall, 11.7% of patients underwent THA conversion within 2 years. The conversion rate was lowest in patients aged younger than 40 years (3.0%) and highest in the 60- to 69-year-old group (35.0%) (P < .001). We found an increased risk of THA conversion in older patients and in patients with osteoarthritis or obesity at the time of hip arthroscopy. Patients treated at high-volume hip arthroscopy centers had a lower THA conversion rate than those treated at low-volume centers (15.1% v 9.7%, P < .001).Conclusions: Hip arthroscopy is performed in patients of various ages, including middle-aged and elderly patients. Older patients have a higher rate of conversion to THA, as do patients with osteoarthritis or obesity.Level Of Evidence: Level III, retrospective comparative study. [ABSTRACT FROM AUTHOR]

Published

2016

36. A concise evidence-based physical examination for diagnosis of acromioclavicular joint pathology: a systematic review

Author

Krill, Michael K., Rosas, Samuel, Kwon, KiHyun, Dakkak, Andrew, Nwachukwu, Benedict U., and McCormick, Frank

Abstract

ABSTRACTObjectives: The clinical examination of the shoulder joint is an undervalued diagnostic tool for evaluating acromioclavicular (AC) joint pathology. Applying evidence-based clinical tests enables providers to make an accurate diagnosis and minimize costly imaging procedures and potential delays in care. The purpose of this study was to create a decision tree analysis enabling simple and accurate diagnosis of AC joint pathology.Methods: A systematic review of the Medline, Ovid and Cochrane Review databases was performed to identify level one and two diagnostic studies evaluating clinical tests for AC joint pathology. Individual test characteristics were combined in series and in parallel to improve sensitivities and specificities. A secondary analysis utilized subjective pre-test probabilities to create a clinical decision tree algorithm with post-test probabilities.Results: The optimal special test combination to screen and confirm AC joint pathology combined Paxinos sign and O’Brien’s Test, with a specificity of 95.8% when performed in series; whereas, Paxinos sign and Hawkins-Kennedy Test demonstrated a sensitivity of 93.7% when performed in parallel. Paxinos sign and O’Brien’s Test demonstrated the greatest positive likelihood ratio (2.71); whereas, Paxinos sign and Hawkins-Kennedy Test reported the lowest negative likelihood ratio (0.35).Conclusion: No combination of special tests performed in series or in parallel creates more than a small impact on post-test probabilities to screen or confirm AC joint pathology. Paxinos sign and O’Brien’s Test is the only special test combination that has a small and sometimes important impact when used both in series and in parallel. Physical examination testing is not beneficial for diagnosis of AC joint pathology when pretest probability is unequivocal. In these instances, it is of benefit to proceed with procedural tests to evaluate AC joint pathology. Ultrasound-guided corticosteroid injections are diagnostic and therapeutic. An ultrasound-guided AC joint corticosteroid injection may be an appropriate new standard for treatment and surgical decision-making.Level of Evidence: II – Systematic Review.

Published

2018

37. Drug-tolerant persister cancer cells are vulnerable to GPX4 inhibition

Author

Hangauer, Matthew J., Viswanathan, Vasanthi S., Ryan, Matthew J., Bole, Dhruv, Eaton, John K., Matov, Alexandre, Galeas, Jacqueline, Dhruv, Harshil D., Berens, Michael E., Schreiber, Stuart L., McCormick, Frank, and McManus, Michael T.

Abstract

Cancer persister cells, which survive cytotoxic treatments, are shown to be sensitive to inhibition of the lipid hydroperoxidase GPX4.

Published

2017

38. Farnesyltransferase-Mediated Delivery of a Covalent Inhibitor Overcomes Alternative Prenylation to Mislocalize K-Ras

Author

Novotny, Chris J., Hamilton, Gregory L., McCormick, Frank, and Shokat, Kevan M.

Abstract

Mutationally activated Ras is one of the most common oncogenic drivers found across all malignancies, and its selective inhibition has long been a goal in both pharma and academia. One of the oldest and most validated methods to inhibit overactive Ras signaling is by interfering with its post-translational processing and subsequent cellular localization. Previous attempts to target Ras processing led to the development of farnesyltransferase inhibitors, which can inhibit H-Ras localization but not K-Ras due to its ability to bypass farnesyltransterase inhibition through alternative prenylation by geranylgeranyltransferase. Here, we present the creation of a neo-substrate for farnesyltransferase that prevents the alternative prenlation by geranylgeranyltransferase and mislocalizes oncogenic K-Ras in cells.

Published

2017

39. Trends in sports-related concussion diagnoses in the USA: a population-based analysis using a private-payor database

Author

Amoo-Achampong, Kelms, Rosas, Samuel, Schmoke, Nicholas, Accilien, Yves-Dany, Nwachukwu, Benedict U., and McCormick, Frank

Abstract

ABSTRACTObjective: To describe recent epidemiological trends in concussion diagnosis within the United States (US) population.Methods: We conducted a retrospective review of PearlDiver, a private-payor insurance database. Our search included International Classification of Disease, Ninth Revision codes for sports-related concussions spanning 2010 through 2014. Overall study population included patients aged 5 to 39 with subgroup analysis performed on Cohort A (Youth), children and adolescents aged 5 to 19, and Cohort B (Adults), adults aged 20 to 39. Incidence was defined as the number of individuals diagnosed normalized to the number of patients in the database for each demographic.Results: Our search returned 1,599 patients diagnosed during the study period. The average (±SD) annual rate was 4.14 ± 1.42 per 100,000 patients for the overall population. Youth patients were diagnosed at a mean annual rate of 3.78 ± 1.30 versus 0.36 ± 0.16 per 100,000 in Adults. Concussion normalized incidence significantly increased from 2.47 to 3.87 per 100,000 patients (57%) in the Youth cohort (p = 0.048). In Adults, rate grew from 0.34 to 0.44 per 100,000 patients (29%) but was not statistically significant (p = 0.077). Four-year compound annual growth rates for Youth and Adults were 26.3% and 20.4%, respectively. Youth patients comprised 1,422/1,599 (90.18%) of all concussion diagnoses and were predominantly male (75%). Adults also constituted 138/1,599 (8.63%) of the sample and were also largely male (80%). Midwestern states had highest diagnostic rates (Cohort A:19 per 100,000 and Cohort B:1.8 per 100,000). Both cohorts had the most total diagnoses made in the fourth quarter followed by the second quarter.Conclusion: Sports-related concussion diagnostic rates have grown significantly in the youth population. Quarterly, regional and gender distributions appear consistent with participation in concussion-prone sports. Utilization of individualized and multifaceted approaches are recommended to advance diagnosis, assessment and management of concussions in the U.S. population.

Published

2017

40. Current concepts on the use of corticosteroid injections for knee osteoarthritis.

Author

Law, Tsun Yee, Nguyen, Chau, Frank, Rachel M., Rosas, Samuel, and McCormick, Frank

Abstract

Intraarticular corticosteroid injections are commonly used by the primary care providers and orthopedic surgeons to treat knee pain associated with osteoarthritis (OA). There is a spectrum of options for treating knee OA, ranging from ice therapy to partial or total knee replacement surgery. In mid-range treatment spectrum are different kinds of injections, with the most widely used being corticosteroid and hyaluronic acid. In addition, there are different types of corticosteroids used and also commonly mixed with different local anesthetics. The purpose of this paper is address current concepts on the use of corticosteroid steroid therapy for the treatment of knee OA. [ABSTRACT FROM PUBLISHER]

Published

2015

41. Trends in Meniscal Allograft Transplantation in the United States, 2007 to 2011.

Author

Cvetanovich, Gregory L., Yanke, Adam B., McCormick, Frank, Bach, Bernard R., and Cole, Brian J.

Abstract

Purpose The purpose of this study was to investigate the incidence of meniscal allograft transplantation (MAT) in the United States from 2007 to 2011 and to analyze trends in MAT using a large database of privately insured non-Medicare patients. Methods Patients who underwent MAT (Current Procedural Terminology [CPT] code 29868) from 2007 to 2011 were identified using the PearlDiver Private Payer Database. Demographic and use data available in the database were extracted for patients who underwent MAT. Statistical analysis involved Student t tests, χ-square tests, and linear regression analyses, with statistical significance set at P < .05. Results The PearlDiver database allowed analysis of approximately 25.4 million patients per year during the years 2007 to 2011 (approximately 9% of the US population younger than 65 years). From 2007 to 2011, there were a total of 302 MAT procedures, for an incidence of 0.24 MAT procedures per year per 100,000 patients. There was no statistically significant increase in MAT procedures over time ( P = .36). There was a higher incidence of MAT in male patients (0.26) than in female patients (0.19) ( P = .001). There was a higher incidence of MAT in patients aged 25 to 34 years (0.40) and in those younger than 25 years (0.30) compared with older patients ( P < .001), with 9.7% of MAT procedures being performed in patients younger than age 35 years. Conclusions MAT was an uncommon procedure, with no change in its incidence from 2007 to 2011. MAT procedures were performed more commonly in patients younger than 35 years and in male patients. Level of Evidence Level IV, descriptive epidemiology study. [ABSTRACT FROM AUTHOR]

Published

2015

42. State-of-the-art anterior cruciate ligament tears: A primer for primary care physicians.

Author

Salzler, Matt, Nwachukwu, Benedict U., Rosas, Samuel, Chau Nguyen, Tsun Yee Law, Eberle, Thomas, and McCormick, Frank

Abstract

The purpose of this article is to provide primary care physicians and other members of the medical community with an updated, general review on the subject of anterior cruciate ligament (ACL) tears. We aim to enhance awareness of these injuries and to prepare those practicing in the primary care setting to address these injuries. Because ACL injuries are quite common, it is very likely that a primary care physician will encounter these injuries and need to address them acutely. The current literature is replete with new concepts and controversies regarding ACL injuries, and this article provides a concise review for our target audience in regard to the care of a patient with an ACL injury. This article is composed of an overview with current epidemiologic data, basic anatomy and physiology, clinical presentation, physical examination findings, imaging modalities, and treatment options. After reading this short article, a medical care provider should understand ACL injuries and their appropriate management. [ABSTRACT FROM AUTHOR]

Published

2015

43. Postoperative Rotator Cuff Repair Rehabilitation and Complication Management.

Author

McCormick, Frank, Wilcox III, Reginald B., and Alqueza, Arnold

Abstract

Selection and management of a postoperative rotator cuff repair rehabilitation protocol is a vital component in achieving pain control in patients, a reliable return to activities and preinjury level, retear risk management, and overall surgical outcome. Optimal treatment approaches require a team effort; open communication between the surgeon, the therapist, and the patient; continual reassessment; and a stepwise staged protocol progression. Much work has been done to identify high-level evidence-based rotator cuff rehabilitation protocols and identify risk factors for complications and tendon failure. The orthopedic surgeon is best positioned to identify predictive factors at the time of treatment that influence overall outcome and may direct and customize early rehabilitation based on these assessments. In addition, the surgeon is overall responsible for much of the postoperative decision making: ensuring an optimal environment for tendon healing, avoidance of postoperative stiffness, return to work or activity pressures, postoperative pain management, cost constraints of therapy, avoidance of revision surgery, and optimization of long-term outcome. Thus, a comprehensive understanding of the rotator cuff repair rehabilitation protocol is requisite. This article aims to review patient and surgical factors to consider in customizing the postoperative rehabilitation protocol, present postoperative assessments to guide surgical recovery and rehabilitation, and provide our current evidence-based rehabilitation protocol. [ABSTRACT FROM AUTHOR]

Published

2015

44. Phosphoproteomics in Drug Discovery and Development.

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, Moran, Michael F., Marto, Jarrod A., Brame, Cynthia J., Ornatsky, Olga, Ross, Mark M., Toledo-Sherman, Leticia M., Castro, Alfredo C., Larsen, Brett, Duewel, Henry, Hosfield, Christopher, Orsi, Christopher, Topaloglou, Thodoros, Figeys, Daniel, Caldwell-Busby, Jennifer A., and Stover, David R.

Abstract

The control of enzyme activity by reversible phosphorylation and the role of protein kinases in signal transduction illustrate well the pivotal role of protein phosphorylation in cell regulation. There are numerous examples of the role of protein kinases and phosphatases in disease, and protein kinases in particular are now established as druggable therapeutic targets (1). Phosphoproteomics includes the large-scale determination of protein phosphorylation in cells and tissue, sometimes referred to as phosphoprofiling. Phosphoprofiling is a global approach that can be used to characterize biological states including therapeutic responses. It is augmented by another proteomic method, protein kinase (and protein phosphatase) interaction mapping, which together have the potential—yet to be fully realized—to provide comprehensive pictures of cellular states. A particular utility for these methods will be in drug discovery and development. [ABSTRACT FROM AUTHOR]

Published

2006

45. Structural Biology of Protein Tyrosine Kinases.

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, Cowan-Jacob, Sandra W., Ramage, Paul, Stark, Wilhelm, Fendrich, Gabriele, and Jahnke, Wolfgang

Abstract

Structural understanding of protein tyrosine kinases (PTKs) has significantly progressed during the past 3 to 5 yr. Three-dimensional structures of several PTKs are now available, in both phosphorylated or nonphosphorylated forms, active or inactive states, unliganded or complexed to substrate analogs or inhibitors, and with only the catalytic domain present or in a multidomain construct including Src homology domain (SH)3 and SH2 domains. Detailed knowledge about the structural basis for kinase activity and regulation has been gained, and the structures are widely used for drug design. [ABSTRACT FROM AUTHOR]

Published

2006

46. Testing of Signal Transduction Inhibitors in Animal Models of Cancer.

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, O'Reilly, Terence, and Cozens, Robert

Abstract

Animal models of human disease are used to investigate, describe, explain, and predict biological phenomena and drug effects. In vitro studies provide important information on the potency and spectrum of activity of new compounds by focusing on their interaction with molecular targets in cell-free, cellular, or tissue-based systems. However, in vivo testing exposes compounds to a variety of host factors and allows for potential interaction with other targets than those selectively tested in vitro. Thus it may not be surprising that many agents active in vitro are inactive or deviant from expectations in vivo. Animal models have been extensively used in the preclinical testing of novel anticancer compounds (1-8), and they remain crucial for determining the safety of novel agents (9,10). In the space available it is impossible, and probably not desirable, to try to describe all the tumor models that have been used for testing kinase inhibitors. We will concentrate on some general principles that we have applied and illustrate some of the points by specific examples. Many of these principles not only will apply to the testing of kinase inhibitors; they can equally be applied, after suitable adaptation, to testing of many anti-tumor agents. Indeed, the generalities rather than the specifics probably apply to the testing of agents for many diseases. The focus will be on the preclinical profiling of epidermal growth factor receptor (EGFR) inhibitors in animal models, many of which are in advanced clinical testing (for general reviews, see refs. 11-15). Specific reviews are available on the development of erlotinib (16,17) and gefitinib (18). [ABSTRACT FROM AUTHOR]

Published

2006

47. Glivec® (Gleevec®, Imatinib, STI571).

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, Buchdunger, Elisabeth, and Capdeville, Renaud

Abstract

Chronic myelogenous leukemia (CML) is a clonal hematological disorder characterized by a reciprocal translocation between chromosomes 9 and 22 (1, 2) known as the Philadelphia (Ph) chromosome. The molecular consequence of this interchromosomal exchange is the creation of the bcr-abl gene coding for a protein with elevated tyrosine kinase activity. The demonstration that the expression of Bcr-Abl is both necessary and sufficient to cause a CML-like syndrome in murine bone marrow transplantation models (3-5) and the finding that the tyrosine kinase activity of Bcr-Abl is crucial for its transforming activity (6), has established the enzymatic activity of this deregulated protein as an attractive drug target addressing Bcr-Abl-positive leukemias. For the first time, a drug target was identified that very clearly differed in its activity between normal and leukemic cells. It was conceivable that this enzyme could be approached with classical tools of pharmacology since its activity, the transfer of phosphate from adenosine triphosphate (ATP) to tyrosine residues of protein substrates, could clearly be described and measured in biochemical as well as cellular assays. Furthermore, cell lines were available that were derived from human leukemic cells that had the same chromosomal abnormality. Such cell lines were instrumental for in vitro and animal studies that laid the groundwork for the clinical trials. So, the essential tools were assembled to go forward aiming at identifying potent and selective inhibitors of the Abl tyrosine kinase. [ABSTRACT FROM AUTHOR]

Published

2006

48. Platelet-Derived Growth Factor.

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, Sjöblom, Tobias, Pietras, Kristian, östman, Arne, and Heldin, Carl-Henrik

Abstract

Platelet-derived growth factor (PDGF) is a family of isoforms that stimulate the growth, survival, and motility of fibroblasts, smooth muscle cells, and other cell types (reviewed in ref. 1) (Fig. 1). PDGF was originally identified in human platelets and purified from this source; however, subsequent studies have shown that PDGF is synthesized by a number of different cell types. [ABSTRACT FROM AUTHOR]

Published

2006

49. JAK Kinases in Leukemias, Lymphomas, and Multiple Myeloma.

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, Burger, Renate, and Gramatzki, Martin

Abstract

The Janus kinase or just another kinase (JAK) family comprises cytoplasmic receptor-associated protein tyrosine kinases that are involved in signal transduction pathways mediated by many cytokines and cytokine-like hormones (1-4). Physiologically, these cytokines play a critical role in regulating normal cellular functions such as proliferation, survival, and differentiation. The importance of JAKs derives from the fact that they are the first proteins involved in the intracellular part of cytokine-induced signal transduction. The major signaling events downstream of JAKs are the activation of the signal transducer and activator of transcription (STAT) proteins, the Ras/Raf/mitogen-activated protein kinase (MAPK), and the phosphatidylinositol-3 kinase (PI3-K)/Akt pathways (5). Dysregulated JAK activity has pathological implications: constitutive or enhanced JAK activation has been implicated in neoplastic transformation and abnormal cell proliferation in various hematological malignancies including multiple myeloma. Therefore, JAKs represent an attractive target for the development of novel drugs that might selectively inhibit their activity. Although exciting breakthroughs have been achieved with other tyrosine kinase inhibitors, such as STI571/imatinib mesylate, pharmacological JAK inhibitors have not yet reached the clinical stage. This chapter focuses on what is known on the role of JAKs in hematological malignancies including multiple myeloma, and the development of pharmacological inhibitors for therapy of diseases associated with JAK activity. [ABSTRACT FROM AUTHOR]

Published

2006

50. Activated FLT3 Receptor Tyrosine Kinase as a Therapeutic Target In Leukemia.

Author

Teicher, Beverly A., Fabbro, Doriano, McCormick, Frank, Scheijen, Blanca, and Griffin, James D.

Abstract

Acute myeloid leukemia (AML) is a heterogeneous neoplastic disease characterized by deregulated proliferation of myeloid precursor cells combined with an arrest in the differentiation process. The abnormal survival advantage of transformed immature myeloid precursors further contributes to a marked impairment of the functional maturation of the various myeloid cell lineages. Intensive studies over the past 20 yr have resulted in the identification of leukemia-specific cytogenetic abnormalities, which provided considerable insight into the underlying pathogenesis of AML. This has also resulted in the prognostic stratification of AML patients into three different risk groups: those with favorable, intermediate or standard, and poor risk disease. Patients with favorable cytogenetics, i.e., those with translocations t(15;17), t(8;21), and inversion inv(16), have particularly benefited from an improved understanding of the molecular pathology of their disease, which has resulted in the identification of potential therapeutic targets. For example, the addition of all-trans retinoic acid during induction chemotherapy for acute promyelocytic leukemia (APL) patients with the PML/RARα (promyelocytic leukemia/retinoic acid receptor-α) fusion gene in t(15;17) has increased the 5-yr survival a further 20-30% compared with chemotherapy alone (1,2). [ABSTRACT FROM AUTHOR]

Published

2006