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2. An evaluation of anaesthetic waste generation at a Johannesburg academic hospital.

Author

Meintjes, J. and Gilliland, L.

Subjects
*MEDICAL wastes, *INCINERATION, *WASTE recycling, *WASTE management, *GLOBAL warming
Abstract

Background: The healthcare sector contributes directly to global warming and environmental decline. This is partly due to disproportionately large waste generation compared to other sectors and the environmental consequences of medical waste incineration. Waste separation and recycling decrease the total waste generation of the theatre complex, decreasing the cost of waste disposal, and if properly implemented, can generate revenue. Waste separation is not performed uniformly, and no recycling programmes exist in the theatre complexes of the academic hospitals in Johannesburg. Potentially recyclable anaesthetic waste is not identified in our setting. Methods: Recyclable anaesthetic waste items were identified. Anaesthetic waste was collected after every anaesthetic case. General and medical waste were weighed respectively and inspected for correct separation. Recyclable items were separated from general waste and weighed. Results: A total of 107.6 kg of anaesthetic waste was evaluated. Per anaesthetic case, 74.6% (65.0-84.2%) was medical waste, and 25.4% (15.8-35.0%) was general waste. Of the general waste, 68.8% (57.7-78.8%) was recyclable. Only 6.8% of medical and 61.4% of general waste bags inspected were correctly separated. Within each medical waste bag, 6.9% (2.3-15.5%) of waste was incorrectly placed general waste. Similarly, each general waste bag contained 6% (0-21.6%) incorrectly placed medical waste. Waste generated per surgical discipline was significantly different. Conclusion: Correct waste separation, a key step in decreasing the burden of healthcare waste, was poor. The study demonstrated that most general anaesthetic waste is recyclable. [ABSTRACT FROM AUTHOR]

Published
2024
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3. An audit of anaesthetic charts at Chris Hani Baragwanath Academic Hospital

Author

Nkadimeng, LM, Gilliland, L, Nel, D, and Mashinini, M

Subjects
anaesthesia, audit, anaesthetic charts
Abstract

Background: The anaesthetic chart is an important component of a patient’s health record in the perioperative period. Studies have shown that anaesthetic charts are often incomplete. The adequacy of chart completion in the anaesthetic department at Chris Hani Baragwanath Academic Hospital (CHBAH) has never been quantified. An audit was done, and the charts were assessed for adequacy of completion.Methods: This audit assessed adequacy of completion of anaesthetic charts for 2019. Using a peer-reviewed checklist adapted from guidelines by the Australian and New Zealand College of Anaesthetists (ANZCA) and the South African Society of Anaesthesiologists (SASA). A sample of 333 charts was audited to assess adequacy of completion. To eliminate sampling bias, a stratified sampling method was used.Results: Completeness was defined as a chart scoring 100%. None of the charts, however, scored 100% and the overall median score was 77%. Charts were subdivided into three groups. Those scoring 75–99% (n = 212), those scoring 50–74% (n = 121) and those that were less than 50% complete (n = 0). Patient category (adult vs paediatrics), time of shift (day vs night) and type of anaesthetic were audited and compared as factors that could affect chart completeness. The only factor that had a statistically significant difference in chart completeness was the patient category, where adult chart completion scored higher compared to paediatric charts, with a p-value < 0.0074.Conclusion: The audited charts scored higher than charts in previous audits done both locally and internationally. Some important aspects of the charts were poorly documented. Ongoing audits and training on chart completion can potentially improve the adequacy of completion and should be part of the academic programme. Better documentation could potentially lead to improved perioperative patient care and mitigate medicolegal risks.

Published
2023

5. The effects of anatomical errors on shoulder kinematics computed using multi-body models

Author

Lavaill, M, Martelli, S, Gilliland, L, Gupta, A, Kerr, G, Pivonka, P, Lavaill, M, Martelli, S, Gilliland, L, Gupta, A, Kerr, G, and Pivonka, P

Abstract

Joint motion calculated using multi-body models and inverse kinematics presents many advantages over direct marker-based calculations. However, the sensitivity of the computed kinematics is known to be partly caused by the model and could also be influenced by the participants' anthropometry and sex. This study aimed to compare kinematics computed from an anatomical shoulder model based on medical images against a scaled-generic model and quantify the effects of anatomical errors and participants' anthropometry on the calculated joint angles. Twelve participants have had planar shoulder movements experimentally captured in a motion lab, and their shoulder anatomy imaged using an MRI scanner. A shoulder multi-body dynamics model was developed for each participant, using both an image-based approach and a scaled-generic approach. Inverse kinematics have been performed using the two different modelling procedures and the three different experimental motions. Results have been compared using Bland-Altman analysis of agreement and further analysed using multi-linear regressions. Kinematics computed via an anatomical and a scaled-generic shoulder models differed in average from 3.2 to 5.4 degrees depending on the task. The MRI-based model presented smaller limits of agreement to direct kinematics than the scaled-generic model. Finally, the regression model predictors, including anatomical errors, sex, and BMI of the participant, explained from 41 to 80% of the kinematic variability between model types with respect to the task. This study highlighted the consequences of modelling precision, quantified the effects of anatomical errors on the shoulder kinematics, and showed that participants' anthropometry and sex could indirectly affect kinematic outcomes.

Published
2022

6. An audit of anaesthetic charts at Chris Hani Baragwanath Academic Hospital.

Author

Nkadimeng, L. M., Gilliland, L., Nel, D., and Mashinini, M.

Subjects
*ANESTHETICS, *AUDITING, *PERIOPERATIVE care, *HOSPITALS, *ANESTHESIOLOGISTS
Abstract

Background: The anaesthetic chart is an important component of a patient’s health record in the perioperative period. Studies have shown that anaesthetic charts are often incomplete. The adequacy of chart completion in the anaesthetic department at Chris Hani Baragwanath Academic Hospital (CHBAH) has never been quantified. An audit was done, and the charts were assessed for adequacy of completion. Methods: This audit assessed adequacy of completion of anaesthetic charts for 2019. Using a peer-reviewed checklist adapted from guidelines by the Australian and New Zealand College of Anaesthetists (ANZCA) and the South African Society of Anaesthesiologists (SASA). A sample of 333 charts was audited to assess adequacy of completion. To eliminate sampling bias, a stratified sampling method was used. Results: Completeness was defined as a chart scoring 100%. None of the charts, however, scored 100% and the overall median score was 77%. Charts were subdivided into three groups. Those scoring 75–99% (n = 212), those scoring 50–74% (n = 121) and those that were less than 50% complete (n = 0). Patient category (adult vs paediatrics), time of shift (day vs night) and type of anaesthetic were audited and compared as factors that could affect chart completeness. The only factor that had a statistically significant difference in chart completeness was the patient category, where adult chart completion scored higher compared to paediatric charts, with a p-value < 0.0074. Conclusion: The audited charts scored higher than charts in previous audits done both locally and internationally. Some important aspects of the charts were poorly documented. Ongoing audits and training on chart completion can potentially improve the adequacy of completion and should be part of the academic programme. Better documentation could potentially lead to improved perioperative patient care and mitigate medicolegal risks. [ABSTRACT FROM AUTHOR]

Published
2022
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7. Toward surgical resilience.

Author

Gilliland, L.

Subjects
*PREHABILITATION, *SURGERY
Abstract

Prehabilitation consists of planned interventions implemented prior to surgery with the aim of increasing functional reserve and creating surgical resilience to positively impact a patient's surgical outcome. [ABSTRACT FROM AUTHOR]

Published
2022
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8. Heart failure for the anaesthetist.

Author

Gilliland, L.

Subjects
*HEART failure, *ANESTHESIOLOGISTS, *HEART failure patients, *RISK assessment
Abstract

Patients with heart failure have increased risk for adverse cardiac events including death, following non-cardiac surgery. The necessity of surgery needs to be determined along with appropriate preoperative evaluation and risk stratification. The anaesthetic should be tailored to specific haemodynamic goals with careful fluid management and appropriate use of vasoactive therapies. [ABSTRACT FROM AUTHOR]

Published
2021
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11. You beta block: or not?

Author

Gilliland, L.

Subjects
*MYOCARDIUM, *BLOOD vessels, *SMOOTH muscle, *CATECHOLAMINES
Abstract

β-blockers bind selectively to beta-adrenergic receptors and interfere with catecholamines provoking β-responses on the heart and smooth muscles of the airways and blood vessels. To block or not to block. [ABSTRACT FROM AUTHOR]

Published
2020
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19. Activation of murine T-cells via phospholipase-C gamma 1-associated protein tyrosine phosphorylation is reduced with aging.

Author

Grossmann, A, Rabinovitch, P S, Kavanagh, T J, Jinneman, J C, Gilliland, L K, Ledbetter, J A, and Kanner, S B

Abstract

Cross-linking of the T-cell receptor (CD3) induces activation of tyrosine kinases and the subsequent phosphorylation of intracellular protein substrates. We examined whether early events in signal transduction through CD3 or CD3 x CD4 receptor ligation were altered in aged murine T-lymphocytes. Both calcium mobilization and tyrosine phosphorylation of phospholipase C gamma 1 (PLC gamma 1) were decreased in T-lymphocytes from old mice. In addition, there was less tyrosine phosphorylation of a 35/36 kDa protein both in whole cell lysates and in PLC gamma 1 immunoprecipitates from old mice. This 35/36 kDa phosphoprotein binds specifically to the SH2 domains of PLC gamma 1. Using a fusion protein containing the SH2 domains of PLC gamma 1 and human IgG1 heavy chain, we identified three additional proteins that bind to the SH2 domains which were tyrosine phosphorylated following CD3 x CD4 ligation to a lesser degree with age. The tyrosine phosphorylation of two phosphoproteins binding to a fusion protein consisting of the SH2 domains of GAP (ras GTPase-activating protein) and human IgG1 heavy chain was also reduced with aging. The observed binding to SH2 domains was thiol redox sensitive. Thus, decreases in antioxidants with age may be responsible for inhibitory effects on PLC gamma 1-phosphatidylinositol signaling through redox regulation of tyrosine phosphoproteins. [ABSTRACT FROM AUTHOR]

Published
1995
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21. Obituaries.

Author

Edmondson C, Gilliland L, Quenby J, Haig J, Hornby J, Manson L, Davies L, and Nicholls J

Published
2008

22. Universal bispecific antibody for targeting tumor cells for destruction by cytotoxic T cells.

Author

Gilliland, L K, Clark, M R, and Waldmann, H

Abstract

Previous studies have demonstrated that bispecific hybrid antibodies produced by cell-cell fusion or chemically conjugated heteroaggregates can direct cytotoxic T lymphocytes to kill target cells for which they have no intrinsic specificity, a phenomenon we call effector cell retargeting (ECR). These studies used bispecific reagents with one specificity directed to CD3 or Ti on the effector cell and the other directed to a target cell antigen. To avoid the need to create different hybrid hybridomas for each target antigen we have developed a universal means to elicit ECR through the use of an antiglobulin step. We have constructed a bispecific hybrid antibody with dual specificity for CD3 and a rat immunoglobulin light chain allotype. This bispecific antibody could mediate ECR to a range of target cells, each coated with distinct surface-binding rat monoclonal antibodies. A particular advantage of targeting to surface-bound monoclonal antibodies is that all other available effector systems may also attack the same antibody-coated target cell.

Published
1988
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28. Allograft Prosthetic Composite (APC) for Proximal Humeral Bone Deficiency in Revision Reverse Shoulder Arthroplasty: A Technical Note and Systematic Review.

Author

Kang HW, Child C, Italia K, Karel M, Gilliland L, Ingoe H, Maharaj J, Whitehouse S, Cutbush K, and Gupta A

Abstract

Background : Proximal humeral bone deficiency in revision shoulder arthroplasty is an emerging and challenging problem as the use of reverse shoulder arthroplasty (RSA) increases. This paper presents a technical note discussing our detailed preoperative planning steps, surgical techniques, and their rationale in carrying out the use of an allograft prosthetic composite (APC) to address proximal humeral bone deficiency in revision RSA. The outcomes of this technique are also presented. This paper also presents a systematic review to further discuss the existing literature on RSA with APCs. Methods : The preoperative surgical planning and the surgical technique employed to execute proximal humeral reconstruction using APC during revision arthroplasty are discussed in the technical note. The preliminary clinical and radiological results of five patients who underwent revision shoulder arthroplasty with proximal humeral reconstruction using APCs are presented. The PRISMA guidelines were followed to perform the systematic review. A systematic search using PubMed, Embase, and Cochrane databases was conducted. All studies involving RSA and APCs were pooled, and the data were extracted and analyzed. Results : A total of 14 studies were eligible for inclusion in the systematic review, with a total of 255 patients and a mean follow-up of 57 months. All studies in the systematic review and the patients included in the author's case series showed improvements in the level of pain, range of motion, function, and satisfaction. Graft incorporation in the systematic review was 84%. Conclusions : Based on the available literature and the results of our case series, the use of an APC construct is a viable option for proximal humeral bone deficiency in revision shoulder arthroplasty.

Published
2024
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29. Comprehensive review of deep learning in orthopaedics: Applications, challenges, trustworthiness, and fusion.

Author

Alzubaidi L, Al-Dulaimi K, Salhi A, Alammar Z, Fadhel MA, Albahri AS, Alamoodi AH, Albahri OS, Hasan AF, Bai J, Gilliland L, Peng J, Branni M, Shuker T, Cutbush K, Santamaría J, Moreira C, Ouyang C, Duan Y, Manoufali M, Jomaa M, Gupta A, Abbosh A, and Gu Y

Subjects
Humans, Deep Learning, Orthopedics methods
Abstract

Deep learning (DL) in orthopaedics has gained significant attention in recent years. Previous studies have shown that DL can be applied to a wide variety of orthopaedic tasks, including fracture detection, bone tumour diagnosis, implant recognition, and evaluation of osteoarthritis severity. The utilisation of DL is expected to increase, owing to its ability to present accurate diagnoses more efficiently than traditional methods in many scenarios. This reduces the time and cost of diagnosis for patients and orthopaedic surgeons. To our knowledge, no exclusive study has comprehensively reviewed all aspects of DL currently used in orthopaedic practice. This review addresses this knowledge gap using articles from Science Direct, Scopus, IEEE Xplore, and Web of Science between 2017 and 2023. The authors begin with the motivation for using DL in orthopaedics, including its ability to enhance diagnosis and treatment planning. The review then covers various applications of DL in orthopaedics, including fracture detection, detection of supraspinatus tears using MRI, osteoarthritis, prediction of types of arthroplasty implants, bone age assessment, and detection of joint-specific soft tissue disease. We also examine the challenges for implementing DL in orthopaedics, including the scarcity of data to train DL and the lack of interpretability, as well as possible solutions to these common pitfalls. Our work highlights the requirements to achieve trustworthiness in the outcomes generated by DL, including the need for accuracy, explainability, and fairness in the DL models. We pay particular attention to fusion techniques as one of the ways to increase trustworthiness, which have also been used to address the common multimodality in orthopaedics. Finally, we have reviewed the approval requirements set forth by the US Food and Drug Administration to enable the use of DL applications. As such, we aim to have this review function as a guide for researchers to develop a reliable DL application for orthopaedic tasks from scratch for use in the market., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published
2024
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30. The Use of Glenoid Structural Allografts for Glenoid Bone Defects in Reverse Shoulder Arthroplasty.

Author

Ingoe H, Italia K, Gilliland L, Kang HW, Karel M, Maharaj J, Cutbush K, and Gupta A

Abstract

Background: The use of reverse shoulder arthroplasty as a primary and revision implant is increasing. Advances in implant design and preoperative surgical planning allow the management of complex glenoid defects. As the demand for treating severe bone loss increases, custom allograft composites are needed to match the premorbid anatomy. Baseplate composite structural allografts are used in patients with eccentric and centric defects to restore the glenoid joint line. Preserving bone stock is important in younger patients where a revision surgery is expected. The aim of this article is to present the assessment, planning, and indications of femoral head allografting for bony defects of the glenoid. Methods: The preoperative surgical planning and the surgical technique to execute the plan with a baseplate composite graft are detailed. The preliminary clinical and radiological results of 29 shoulders which have undergone this graft planning and surgical technique are discussed. Clinical outcomes included visual analogue score of pain (VAS), American Shoulder and Elbow Surgeons score (ASES), Constant-Murley score (CS), satisfaction before and after operation, and active range of motion. Radiological outcomes included graft healing and presence of osteolysis or loosening. Results: The use of composite grafts in this series has shown excellent clinical outcomes, with an overall graft complication rate in complex bone loss cases of 8%. Conclusion: Femoral head structural allografting is a valid and viable surgical option for glenoid bone defects in reverse shoulder arthroplasty.

Published
2024
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31. Restoration of glenoid joint line: a three-dimensional analysis of scapular landmarks.

Author

Gilliland L, Launay M, Salhi A, Green N, Maharaj J, Italia KR, Cutbush K, and Gupta A

Abstract

Background: Restoration of the glenoid joint line in shoulder arthroplasty is important for implant positioning and function. Medialization of the glenohumeral joint line due to glenoid bone loss is commonly encountered in primary and revision of shoulder arthroplasty albeit the direction and location of bone loss varies with different pathology. Three-Dimensional (3D) planning software has assisted in preoperative planning of complex glenoid deformities. However, limited literature is available defining a reliable 3D method to evaluate the glenoid joint line preoperatively., Aims: The purpose of this study is to identify a set of reliable scapular landmarks to be used as reference points to measure the premorbid glenoid joint line using 3D segmented models of healthy scapulae., Methods: Bilateral computed tomography scans from 79 patients eligible for primary stabilization procedures were retrospectively selected from our institutional surgical database (mean age 35 ± 10 years, 58 males and 21 females). 3D models of the contralateral healthy scapulae were created via computed tomography scan segmentation using Mimics 24.0 software (Materialise, Leuven, Belgium). Anatomical landmarks were identified using 3-Matic 16.0 software (Materialise, Leuven, Belgium). The distance between identified landmarks and a sagittal plane created on the deepest point of the glenoid was recorded for each scapula and reliability of each landmark was assessed. Inter- and intra-observer reliabilities were also evaluated using intraclass correlation coefficients (ICCs)., Results: Four landmarks showed statistically significant results: the scapular notch (SN), the centroid of the coracoid (CC), a point on the most medial border of the scapula in line with the scapular spine (TS), and the most lateral point of the acromion (AL). The mean (± standard deviation) joint line measured from the SN, CC, TS and AL were 28.36 ± 2.97 mm, 11.66 ± 2.07 mm, 107.52 ± 8.1 mm, and 29.72 ± 4.46 mm, respectively. Inter-observer reliability analysis for SN, TS, and AL showed excellent agreement with ICC values of 0.966, 0.997, and 0.944, respectively, and moderate agreement for CC with ICC of 0.728., Conclusion: The results from this study assist in estimating joint line medialization preoperatively and in planning its subsequent restoration. A set of reliable landmarks can be used as references to estimate the premorbid glenoid joint line preoperatively., (© 2023 The Author(s).)

Published
2023
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32. Single-Stage Revision Reverse Shoulder Arthroplasty: Preoperative Planning, Surgical Technique, and Mixed Reality Execution.

Author

Italia K, Launay M, Gilliland L, Nielsen J, Pareyon R, Hollman F, Salhi A, Maharaj J, Jomaa M, Cutbush K, and Gupta A

Abstract

Revision shoulder arthroplasty is increasing with the number of primary shoulder replacements rising globally. Complex primary and revisions of shoulder arthroplasties pose specific challenges for the surgeon, which must be addressed preoperatively and intraoperatively. This article aimed to present strategies for the management of revision of shoulder arthroplasties through a single-stage approach. Preoperatively, patient factors, such as age, comorbidities, and bone quality, should be considered. The use of planning software can aid in accurately evaluating implants in situ and predict bony anatomy that will remain after explantation during the revision surgery. The planning from such software can then be executed with the help of mixed reality technology to allow accurate implant placement. Single-stage revision is performed in two steps (debridement as first step, implantation and reconstruction as the second step), guided by the following principles: adequate debridement while preserving key soft tissue attachments (i.e., rotator cuff, pectoralis major, latissimus dorsi, deltoid), restoration of glenoid joint line using bone grafting, restoration of humeral length, reconstruction and/or reattachment of soft tissues, and strict compliance with the postoperative antibiotic regimen. Preliminary results of single-stage revision shoulder arthroplasty show improvement in patient outcomes (mean 1 year), successful treatment of infection for those diagnosed with periprosthetic joint infection, and improved cost-benefit parameters for the healthcare system.

Published
2022
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33. The effects of anatomical errors on shoulder kinematics computed using multi-body models.

Author

Lavaill M, Martelli S, Gilliland L, Gupta A, Kerr G, and Pivonka P

Subjects
Humans, Biomechanical Phenomena, Models, Anatomic, Magnetic Resonance Imaging, Shoulder anatomy & histology, Shoulder Joint
Abstract

Joint motion calculated using multi-body models and inverse kinematics presents many advantages over direct marker-based calculations. However, the sensitivity of the computed kinematics is known to be partly caused by the model and could also be influenced by the participants' anthropometry and sex. This study aimed to compare kinematics computed from an anatomical shoulder model based on medical images against a scaled-generic model and quantify the effects of anatomical errors and participants' anthropometry on the calculated joint angles. Twelve participants have had planar shoulder movements experimentally captured in a motion lab, and their shoulder anatomy imaged using an MRI scanner. A shoulder multi-body dynamics model was developed for each participant, using both an image-based approach and a scaled-generic approach. Inverse kinematics have been performed using the two different modelling procedures and the three different experimental motions. Results have been compared using Bland-Altman analysis of agreement and further analysed using multi-linear regressions. Kinematics computed via an anatomical and a scaled-generic shoulder models differed in average from 3.2 to 5.4 degrees depending on the task. The MRI-based model presented smaller limits of agreement to direct kinematics than the scaled-generic model. Finally, the regression model predictors, including anatomical errors, sex, and BMI of the participant, explained from 41 to 80% of the kinematic variability between model types with respect to the task. This study highlighted the consequences of modelling precision, quantified the effects of anatomical errors on the shoulder kinematics, and showed that participants' anthropometry and sex could indirectly affect kinematic outcomes., (© 2022. The Author(s).)

Published
2022
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34. Imaging and pathologic features of non-calcified ductal carcinoma in situ: can sonography predict upgrade?

Author

Komarla R, Gilliland L, Piraner M, Seidel R, Clifford K, and Kunjummen J

Subjects
Adult, Aged, Aged, 80 and over, Biopsy, Large-Core Needle methods, Cohort Studies, Female, Humans, Image-Guided Biopsy methods, Magnetic Resonance Imaging statistics & numerical data, Mammography statistics & numerical data, Middle Aged, Neoplasm Invasiveness, Retrospective Studies, Breast Neoplasms diagnostic imaging, Breast Neoplasms pathology, Carcinoma, Intraductal, Noninfiltrating diagnostic imaging, Carcinoma, Intraductal, Noninfiltrating pathology, Ultrasonography, Mammary statistics & numerical data
Abstract

Objective: The purpose of this study was to evaluate the imaging and pathologic features and upgrade rate of non-calcified ductal carcinoma in situ (NCDCIS). The study tested the hypothesis that lesions with sonographic findings have higher upgrade rate compared to lesions seen on mammography or MRI only., Methods: This retrospective study included patients with ductal carcinoma in situ (DCIS) diagnosed by image-guided core breast biopsy from December 2009 to April 2018. Patients with microcalcifications on mammography or concurrent ipsilateral cancer on core biopsy were excluded. An upgrade was defined as surgical pathology showing microinvasive or invasive cancer., Results: A total of 71 lesions constituted the study cohort. 62% of cases (44/71) had a mammographic finding, and 38% (27/71) of mammographically occult lesions had findings on either ultrasound, MRI, or both. Of the 67 cases that underwent sonography, a mass was noted in 56/67 (83.6%) cases and no sonographic correlate was identified in 11/67 (16.4%) cases. 21% (15/71) of lesions were upgraded on final surgical pathology. The upgrade rate of patients with sonographic correlate was 27% (15/56) vs with mammographic findings only was 0% (0/11)., Conclusion: DCIS should be considered in the differential diagnosis of architectural distortion, asymmetries, focal asymmetries, and masses, even in the absence of microcalcifications. NCDCIS diagnosed by ultrasound may be an independent risk factor for upgrade., Advances in Knowledge: Radiologists must be aware of imaging features of DCIS and consider increased upgrade rate when NCDCIS is diagnosed by ultrasound.

Published
2022
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35. Radiologists and Social Media: Do Not Forget About Facebook.

Author

Seidel RL, Jalilvand A, Kunjummen J, Gilliland L, and Duszak R Jr

Subjects
Humans, Retrospective Studies, Breast Diseases diagnostic imaging, Radiologists, Social Media statistics & numerical data
Abstract

Purpose: Facebook (Facebook, Inc, Menlo Park, California, USA) is the most popular social networking platform worldwide. Facebook groups are virtual communities of people who share a common interest. Breast Imaging Radiologists is a Facebook group for radiologists with an interest in breast imaging. The purpose of this study was to analyze the membership and activity of the Breast Imaging Radiologists Facebook group (BIRFG) for 2 years since its inception., Methods: Using both the Grytics (www.grytics.com) and Sociograph (www.sociograph.io) analytic engines, the activity of the BIRFG was analyzed retrospectively from its inception on February 11, 2015, through February 12, 2017. Activity data were exported for further qualitative and quantitative analysis using Excel (Microsoft, Redmond, Washington, USA). Member demographic data were obtained by querying public Facebook profiles, US News Doctor Finder (US News & World Report, Washington, DC, USA), Doximity (Doximity, San Francisco, California, USA), and Google (Google Inc, Mountain View, California, USA)., Results: Membership grew from 1 to 774 over the study period, and 84% of the members were female. There were 493 posts, 3,253 comments, and 1,732 reactions; 92% of posts received either comments or reactions. Each post received an average of 6.6 comments, and 55% of members were active over the study period. There was an increase in all measures of activity from year 1 to year 2., Conclusions: Our findings indicate that radiologists find value in using Facebook groups as a forum to network and exchange information about breast imaging. This may be generalizable to other radiology subspecialties. Given the popularity and accessibility of Facebook for personal use, it may prove a more comfortable social medium for radiologists to interact professionally., (Copyright © 2017 American College of Radiology. Published by Elsevier Inc. All rights reserved.)

Published
2018
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36. Front squat data reproducibility collected with a triple-axis accelerometer.

Author

Caruso JF, Olson NM, Taylor ST, McLagan JR, Shepherd CM, Borgsmiller JA, Mason ML, Riner RR, Gilliland L, and Grisewold S

Subjects
Athletes, Football physiology, Humans, Movement physiology, Muscle, Skeletal physiology, Reproducibility of Results, Resistance Training instrumentation, Resistance Training methods
Abstract

The purpose of our study was to assess data reproducibility from 2 consecutive front squat workouts, spaced 1 week apart, performed by American college football players (n = 18) as they prepared for their competitive season. For each workout, our methods entailed the performance of 3-6 front squat repetitions per set at 55, 65, and 75% of subject's 1 repetition maximum (1RM) load. In addition, a fourth set was done at a heavier load, with a resistance equal to 80 and 83% of their 1RM values, for the first and second workouts, respectively. A triple-axis accelerometer was affixed to a barbell to quantify exercise performance. Per load, the accelerometer measures peak values for the following indices: force, velocity, and power. To assess data reproducibility, inter-workout comparisons were made for 12 performance indices with 4 statistical test-retest measures: intraclass correlation coefficients, coefficients of variation (CVs), and the SEM expressed in both absolute and relative terms. Current results show that the majority of performance indices exceeded intraclass correlation (0.75-0.80) and CV (10-15%) values previously deemed as acceptable levels of data reproducibility. The 2 indices with the greatest variability were power and velocity values obtained at 55% of the 1RM load; thus, it was concluded that higher movement rates at the lightest load were the most difficult aspect of front squat performance to repeat successfully over time. Our practical applications imply lighter loads, with inherently higher rates of barbell movement, yield lower data reproducibility values.

Published
2012
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37. Virtual cystoscopy.

Author

Mohammed A, Simpson A, Zamora I, and Gilliland L

Subjects
Humans, Imaging, Three-Dimensional methods, Imaging, Three-Dimensional trends, Software trends, Tomography, X-Ray Computed methods, Tomography, X-Ray Computed trends, Urinary Bladder Neoplasms diagnostic imaging
Abstract

Bladder cancer is a common problem facing urologists worldwide. The gold standard for its diagnosis and follow-up is the direct visualization of the tumor using conventional cystoscopy. Despite having high sensitivity and specificity for detecting bladder cancer, conventional cystoscopy is regarded as an invasive procedure which is associated with several complications. In addition, regular follow-up of patients with bladder cancer is a financial burden on the health system. With the progressive development in diagnostic imaging and medical computer software technologies, it was possible to generate virtual reality images to aid the clinician to inspect the interior of the bladder in real time. This technology is considered as a safe test for bladder cancer diagnosis and follow-up, and it is associated with cancer detection rates comparable with conventional cystoscopy. However, it is associated with some drawbacks that limit its use in routine clinical practice at the current time. In this paper, we review the development and clinical applications of this technology.

Published
2008
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38. STI-HIV prevention: a model program in a school-based health center.

Author

Gilliland L and Scully J

Subjects
Adolescent, Adolescent Behavior psychology, HIV Infections prevention & control, Health Behavior, Humans, Psychology, Adolescent, Self Efficacy, United States, Adolescent Health Services organization & administration, Health Knowledge, Attitudes, Practice, School Health Services organization & administration, School Nursing organization & administration, Sex Education organization & administration, Sexually Transmitted Diseases nursing, Sexually Transmitted Diseases prevention & control
Abstract

Prevention programs are a valuable component of the comprehensive services offered at school-based health centers (SBHC). Reducing risky adolescent behaviors is an effective way to reduce the morbidity and mortality burden among the school-age population. Programs using peer educators and youth-initiated websites can increase knowledge and self-esteem and help reduce risky sexual behaviors. Because many SBHCs provide services beyond traditional primary care, there is great need to support and increase the number of SBHC prevention programs targeted at communities at risk.

Published
2005
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39. One plant actin isovariant, ACT7, is induced by auxin and required for normal callus formation.

Author

Kandasamy MK, Gilliland LU, McKinney EC, and Meagher RB

Subjects
Actins biosynthesis, Actins genetics, Antibodies, Monoclonal, Arabidopsis genetics, Arabidopsis metabolism, Culture Techniques, Gene Expression Regulation, Plant, Genetic Complementation Test, Multigene Family, Mutation, Phylogeny, Plant Leaves cytology, Plant Leaves genetics, Plant Proteins, Plant Roots cytology, Plant Roots genetics, Plants, Genetically Modified, Protein Isoforms genetics, Protein Isoforms physiology, Actins physiology, Arabidopsis physiology, Indoleacetic Acids metabolism
Abstract

During plant growth and development, the phytohormone auxin induces a wide array of changes that include cell division, cell expansion, cell differentiation, and organ initiation. It has been suggested that the actin cytoskeleton plays an active role in the elaboration of these responses by directing specific changes in cell morphology and cytoarchitecture. Here we demonstrate that the promoter and the protein product of one of the Arabidopsis vegetative actin genes, ACT7, are rapidly and strongly induced in response to exogenous auxin in the cultured tissues of Arabidopsis. Homozygous act7-1 mutant plants were slow to produce callus tissue in response to hormones, and the mutant callus contained at least two to three times lower levels of ACT7 protein than did the wild-type callus. On the other hand, a null mutation in ACT2, another vegetative actin gene, did not significantly affect callus formation from leaf or root tissue. Complementation of the act7-1 mutants with the ACT7 genomic sequence restored their ability to produce callus at rates similar to those of wild-type plants, confirming that the ACT7 gene is required for callus formation. Immunolabeling of callus tissue with actin subclass-specific antibodies revealed that the predominant ACT7 is coexpressed with the other actin proteins. We suggest that the coexpression, and probably the copolymerization, of the abundant ACT7 with the other actin isovariants in cultured cells may facilitate isovariant dynamics well suited for cellular responses to external stimuli such as hormones.

Published
2001
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40. Elimination of the immunogenicity of therapeutic antibodies.

Author

Gilliland LK, Walsh LA, Frewin MR, Wise MP, Tone M, Hale G, Kioussis D, and Waldmann H

Subjects
Alemtuzumab, Animals, Antibodies, Anti-Idiotypic biosynthesis, Antibodies, Monoclonal administration & dosage, Antibodies, Monoclonal metabolism, Antibodies, Monoclonal, Humanized, Antibodies, Neoplasm administration & dosage, Antibodies, Neoplasm metabolism, Antigens metabolism, Binding Sites, Antibody genetics, Cell Line, Cricetinae, Humans, Immune Tolerance genetics, Immunoglobulin Variable Region chemistry, Immunoglobulin Variable Region genetics, Immunoglobulin Variable Region metabolism, Injections, Intraperitoneal, Lymphocyte Depletion, Mice, Mice, Transgenic, Mutagenesis, Site-Directed, T-Lymphocytes immunology, T-Lymphocytes metabolism, Antibodies, Monoclonal genetics, Antibodies, Monoclonal immunology, Antibodies, Neoplasm genetics, Antibodies, Neoplasm immunology, Protein Engineering methods
Abstract

The immunogenicity of therapeutic Abs limits their long-term use. The processes of complementarity-determining region grafting, resurfacing, and hyperchimerization diminish mAb immunogenicity by reducing the number of foreign residues. However, this does not prevent anti-idiotypic and anti-allotypic responses following repeated administration of cell-binding Abs. Classical studies have demonstrated that monomeric human IgG is profoundly tolerogenic in a number of species. If cell-binding Abs could be converted into monomeric non-cell-binding tolerogens, then it should be possible to pretolerize patients to the therapeutic cell-binding form. We demonstrate that non-cell-binding minimal mutants of the anti-CD52 Ab CAMPATH-1H lose immunogenicity and can tolerize to the "wild-type" Ab in CD52-expressing transgenic mice. This finding could have utility in the long-term administration of therapeutic proteins to humans.

Published
1999

41. Detection of deleterious genotypes in multigenerational studies. I. Disruptions in individual Arabidopsis actin genes.

Author

Gilliland LU, McKinney EC, Asmussen MA, and Meagher RB

Subjects
Alleles, Arabidopsis growth & development, Evolution, Molecular, Gene Frequency, Genotype, Mutagenesis, Insertional, Selection, Genetic, Actins genetics, Arabidopsis genetics, Crosses, Genetic, Mutation genetics
Abstract

Plant actins are involved in numerous cytoskeletal processes effecting plant development, including cell division plane determination, cell elongation, and cell wall deposition. Arabidopsis thaliana has five ancient subclasses of actin with distinct patterns of spatial and temporal expression. To test their functional roles, we identified insertion mutants in three Arabidopsis actin genes, ACT2, ACT4, and ACT7, representing three subclasses. Adult plants homozygous for the act2-1, act4-1, and act7-1 mutant alleles appear to be robust, morphologically normal, and fully fertile. However, when grown as populations descended from a single heterozygous parent, all three mutant alleles were found at extremely low frequencies relative to the wild-type in the F2 generation. Thus, all three mutant alleles appear to be deleterious. The act2-1 mutant allele was found at normal frequencies in the F1, but at significantly lower frequencies than expected in the F2 and F3 generations. These data suggest that the homozygous act2-1/act2-1 mutant adult plants have a reduced fitness in the 2N sporophytic portion of the life cycle, consistent with the vegetative expression of ACT2. These data are interpreted in light of the extreme conservation of plant actin subclasses and genetic redundancy.

Published
1998
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42. Detection of deleterious genotypes in multigenerational studies. II. Theoretical and experimental dynamics with selfing and selection.

Author

Asmussen MA, Gilliland LU, and Meagher RB

Subjects
Arabidopsis genetics, Mathematical Computing, Nonlinear Dynamics, Crosses, Genetic, Genotype, Models, Genetic, Selection, Genetic
Abstract

A mathematical model was developed to help interpret genotype and allele frequency dynamics in selfing populations, with or without apomixis. Our analysis provided explicit time-dependent solutions for the frequencies at diallelic loci in diploid populations under any combination of fertility, viability, and gametic selection through meiotic drive. With no outcrossing, allelic variation is always maintained under gametic selection alone, but with any fertility or viability differences, variation will ordinarily be maintained if and only if the net fitness (fertility x viability) of heterozygotes exceeds that of both homozygotes by a substantial margin. Under pure selfing and Mendelian segregation, heterozygotes must have a twofold fitness advantage; the level of overdominance necessary to preserve genetic diversity declines with apomixis, and increases with segregation distortion if this occurs equally and independently in male and female gametes. A case study was made of the Arabidopsis act2-1 actin mutant over multiple generations initiated from a heterozygous plant. The observed genotypic frequency dynamics were consistent with those predicted by our model for a deleterious, incompletely recessive mutant in either fertility or viability. The theoretical framework developed here should be very useful in dissecting the form(s) and strength of selection on diploid genotypes in populations with negligible levels of outcrossing.

Published
1998
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43. Antibody engineering.

Author

Hayden MS, Gilliland LK, and Ledbetter JA

Subjects
Genetic Engineering, Humans, Immunoglobulins genetics
Abstract

The development of recombinant techniques for the rapid cloning, expression, and characterization of cDNAs encoding antibody (Ab) subunits has revolutionized the field of antibody engineering. By fusion to heterologous protein domains, chain shuffling, and inclusion of self-assembly motifs, novel molecules such as bispecific Abs can now be generated which possess the subset of functional properties designed to fit the intended application. Rapid technological developments in phage display of peptides and proteins have led to a plethora of applications directed towards immunology and antibody engineering. Many of the problems associated with the therapeutic use of Abs are being addressed by the application of these new techniques.

Published
1997
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44. Agonistic activity of a CD40-specific single-chain Fv constructed from the variable regions of mAb G28-5.

Author

Ledbetter JA, Francisco JA, Siegall CB, Gilliland LK, Hollenbaugh D, Aruffo A, Siadak AW, Mischel-Petty N, Grosmaire LS, Gordon ML, Brown TJ, Moran-Davis P, Mittler RS, Kiener PA, and Nadler SG

Subjects
Animals, Antibodies, Monoclonal biosynthesis, Antibodies, Monoclonal genetics, Cells, Cultured, Cloning, Molecular, Endothelium cytology, Gene Expression, Humans, Immunoglobulin Fragments biosynthesis, Immunoglobulin Fragments genetics, Immunoglobulin Variable Region biosynthesis, Immunoglobulin Variable Region genetics, Monocytes immunology, NF-kappa B immunology, Antibodies, Monoclonal immunology, B-Lymphocytes immunology, CD40 Antigens immunology, Immunoglobulin Fragments immunology, Immunoglobulin Variable Region immunology
Abstract

A single-chain Fv (sFv) was expressed from the variable regions of the CD40-specific mAb G28-5. The molecule bound CD40 with a high affinity (2.2 nM) and was a monomer in solution. Surprisingly, G28-5 sFv was a potent CD40 agonist that rapidly crosslinked CD40 on the cell surface but did not crosslink CD40-Ig in solution. G28-5 sFv was a more potent agonist than G28-5 IgG and was able to stimulate CD40 responses by B cells and monocytes. G28-5 IgG partially blocked, whereas G28-5 sFv augmented CD40 responses during stimulation with natural ligand (gp39-CD8 fusion protein). These results indicate that the functional activity of ligands built from the binding site of G28-5 is highly dependent upon the size and physical properties of the molecule both in solution and on the cell surfaces.

Published
1997

45. Fuel identification by neural network analysis of the response of vapor-sensitive sensor arrays.

Author

McCarrick CW, Ohmer DT, Gilliland LA, Edwards PA, and Mayfield HT

Subjects
Chromatography, Gas, Gasoline classification, Gasoline analysis, Neural Networks, Computer
Abstract

Neural network analysis of the response of an array of vapor-sensitive detectors has been used to identify six different types of aviation fuel. The data set included 96 samples of JP-4, JP-5, JP-7, JP-8, JetA, and aviation gasoline (AvGas). A sample of each neat fuel was injected into a continuous stream of breathing air through an injection port from a gas chromatograph. The aspirated sample was then swept from the injection port to the chamber without separation. In the chamber, the sample was exposed to an array of eight vapor-sensitive detectors. The analog output of each detector was digitized and stored while the sample was swept into and through the chamber. The response of each detector was then averaged and stored as the final response or pattern of each sample. It was clear from a visual inspection of each of the radar plots that there was a characteristic pattern in the response of the array to five of the six different fuel types. This was confirmed using neural network analysis to study the entire data set. A two-step procedure was developed to separate the patterns of all six fuel tyes into their respective classes. In the first step, fuels were separated into one of five groups: JP-4, JP-5, JP-7, AvGas, or a combined JP-8/JetA group. In the second step, the fuels in the combined group were separated into either JP-8 or JetA groups.

Published
1996
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46. Specific binding of Fyn and phosphatidylinositol 3-kinase to the B cell surface glycoprotein CD19 through their src homology 2 domains.

Author

Chalupny NJ, Aruffo A, Esselstyn JM, Chan PY, Bajorath J, Blake J, Gilliland LK, Ledbetter JA, and Tepper MA

Subjects
Amino Acid Sequence, Animals, Antigens, CD19 metabolism, Cell Line, Humans, Macromolecular Substances, Mice, Molecular Sequence Data, Peptide Fragments metabolism, Phosphatidylinositol 3-Kinases, Phosphorylation, Protein Binding, Proto-Oncogene Proteins c-fyn, Recombinant Fusion Proteins metabolism, Sequence Alignment, B-Lymphocytes metabolism, Phosphotransferases (Alcohol Group Acceptor) metabolism, Phosphotyrosine metabolism, Protein Processing, Post-Translational, Proto-Oncogene Proteins metabolism, Signal Transduction physiology, src Homology Domains
Abstract

CD19 is a B cell surface protein capable of forming non-covalent molecular complexes with a number of other B cell surface proteins including the CD21/CD81/Leu-13 complex as well as with surface immunoglobulin. CD19 tyrosine phosphorylation increases after B cell activation, and is proposed to play a role in signal transduction through its cytoplasmic domain, which contains nine tyrosine residues. Several second messenger proteins have been shown to immunoprecipitate with CD19, including p59 Fyn (Fyn), p59 Lyn (Lyn) and phosphatidylinositol-3 kinase (PI-3 kinase). These associations are predicted to occur via the src-homology 2 (SH2) domains of the second messenger proteins. Two of the cytoplasmic tyrosines in the CD19 cytoplasmic region contain the consensus binding sequence for the PI-3 kinase SH2 domain (YPO4-X-X-M). However, the reported consensus binding sequence for the Fyn and Lyn SH2 domains (YPO4-X-X-I/L) is not found in CD19. We investigated the capacity of CD19 cytoplasmic tyrosines to bind both Fyn and PI-3 kinase SH2-domain fusion proteins. In activated B cells, both Fyn and PI-3 kinase SH2-domain fusion proteins precipitate CD19. Using synthetic tyrosine-phosphorylated peptides comprising each of the CD19 cytoplasmic tyrosines and surrounding amino acids, we investigated the ability of the Fyn SH2 and PI-3 kinase SH2 fusion proteins to bind to the different CD19 cytoplasmic phosphotyrosine peptides. ELISA revealed that the two CD19 cytoplasmic tyrosine residues contained within the Y-X-X-M sequences (Y484 and Y515) bound preferentially to the PI-3 kinase SH2-domain fusion proteins. Two different tyrosines (Y405 and Y445) bound preferentially to the Fyn SH2-domain fusion protein via a novel sequence, Y-E-N-D/E, different from that previously reported for the Fyn SH2 domain. In precipitation studies, peptide Y484 was able to compete with tyrosine phosphorylated CD19 specifically for binding to the PI-3 kinase SH2 domain fusion proteins, while peptides Y405 and Y445 were able to compete specifically for binding to the Fyn SH2 domain fusion proteins. These results indicate that CD19 may be capable of binding both Fyn and PI-3 kinase concurrently, suggesting a mechanism for CD19 signal transduction, in which binding of PI-3 kinase to the Fyn SH3 domain results in activation of PI-3 kinase.

Published
1995
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47. Activity of a single-chain immunotoxin that selectively kills lymphoma and other B-lineage cells expressing the CD40 antigen.

Author

Francisco JA, Gilliland LK, Stebbins MR, Norris NA, Ledbetter JA, and Siegall CB

Subjects
Antibodies, Monoclonal immunology, Antibodies, Monoclonal isolation & purification, Antibodies, Monoclonal metabolism, Antigens, CD metabolism, Antigens, Differentiation, B-Lymphocyte metabolism, Base Sequence, CD40 Antigens, Cell Death drug effects, Enzyme-Linked Immunosorbent Assay, Epitopes, Humans, Immunoglobulin Heavy Chains immunology, Immunoglobulin Heavy Chains isolation & purification, Immunoglobulin Heavy Chains metabolism, Immunoglobulin Light Chains immunology, Immunoglobulin Light Chains isolation & purification, Immunoglobulin Light Chains metabolism, Immunotoxins isolation & purification, Immunotoxins metabolism, Leukemia, B-Cell metabolism, Leukemia, T-Cell drug therapy, Leukemia, T-Cell immunology, Leukemia, T-Cell pathology, Lymphoma, B-Cell drug therapy, Lymphoma, B-Cell pathology, Lymphoma, T-Cell drug therapy, Lymphoma, T-Cell immunology, Lymphoma, T-Cell pathology, Molecular Sequence Data, Pseudomonas aeruginosa Exotoxin A, ADP Ribose Transferases, Antigens, CD immunology, Antigens, Differentiation, B-Lymphocyte immunology, B-Lymphocytes drug effects, B-Lymphocytes immunology, Bacterial Toxins, Exotoxins toxicity, Immunotoxins toxicity, Leukemia, B-Cell drug therapy, Leukemia, B-Cell immunology, Lymphoma, B-Cell immunology, Virulence Factors
Abstract

We have constructed anti-CD40 immunotoxins consisting of the single chain Fv (sFv) region of the anti-human CD40 mAb G28-5 fused to a truncated form of Pseudomonas exotoxin, PE40. CD40 is an integral membrane glycoprotein found on the surface of B-lineage cells, including lymphomas and leukemias, as well as certain carcinomas. Two forms of the immunotoxin were constructed, one with the light chain variable (VL) region of the sFv preceding the heavy chain variable region (VH) [G28-5 sFv(VL-VH)-PE40] and the second with the sFv in the opposite orientation [G28-5 sFv(VH-VL)-PE40]. Although both forms of G28-5 sFv-PE40 specifically bound to CD40 in ELISAs, the binding of G28-5 sFv(VL-VH)-PE40 was > 10-fold higher. A number of malignant B- and T-cell lines were screened for CD40 expression and susceptibility to G28-5 sFv(VL-VH)-PE40. All of the B-lineage cells tested were CD40 positive and sensitive to the anti-CD40 immunotoxin, with EC50s ranging from 2.5-70 ng/ml, whereas none of the T cell leukemias or lymphomas were antigen positive or were affected by the immunotoxins. Consistent with the antigen-binding results, the VL-VH immunotoxin was > 10-fold more cytotoxic than the VH-VL immunotoxin. The anti-CD40 single-chain immunotoxin fusion protein G28-5 sFv(VL-VH)-PE40 represents a potent and specific cytotoxic agent for the elimination of normal and transformed B-lineage cells expressing CD40.

Published
1995

48. Coengagement of CD2 with LFA-1 or VLA-4 by bispecific ligand fusion proteins primes T cells to respond more effectively to T cell receptor-dependent signals.

Author

Dietsch MT, Chan PY, Kanner SB, Gilliland LK, Ledbetter JA, Linsley PS, and Aruffo A

Subjects
Antibodies, Bispecific, Antigens, CD physiology, CD3 Complex physiology, CD58 Antigens, Calcium metabolism, Humans, Intercellular Adhesion Molecule-1 physiology, Membrane Glycoproteins physiology, Receptor Aggregation, Recombinant Fusion Proteins, Signal Transduction, CD2 Antigens physiology, Lymphocyte Function-Associated Antigen-1 physiology, Receptors, Antigen, T-Cell physiology, Receptors, Very Late Antigen physiology, T-Lymphocytes physiology
Abstract

To examine the effects of ligand engagement and accessory molecule juxtaposition on T cell receptor (TCR) signaling, we prepared LFA-3/ICAM-1 Rg and LFA-3/VCAM-1 Rg bispecific immunoglobulin fusion proteins (Rg, recombinant globulin). These novel fusion proteins allowed us to examine the effects of ligand driven co-engagement of T cell proteins CD2 and LFA-1 or CD2 and VLA-4 on TCR-dependent mobilization of intracellular Ca2+. We observed that preincubation of resting T cells with LFA-3/ICAM-1 Rg or LFA-3/VCAM-1 Rg fusion proteins resulted in significantly enhanced mobilization of intracellular Ca2+ following TCR-accessory molecule cross-linking relative to T cells preincubated with each of the monospecific Rgs alone or with combinations of the monospecific Rg fusion proteins. In addition, such coengagement stimulated TCR-dependent activation and tyrosine phosphorylation of phospholipase C gamma 1 (PLC gamma 1). These results suggest that when T cells interact with antigen presenting cells the engagement of multiple cell adhesion molecules such as CD2, LFA-1, and VLA-4 primes the T cell to respond more effectively to signals delivered through the TCR.

Published
1994
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49. T cell long-term hyporesponsiveness follows antigen receptor engagement and results from defective signal transduction.

Author

Dubois PM, Andris F, Shapiro RA, Gilliland LK, Kaufman M, Urbain J, Ledbetter JA, and Leo O

Subjects
Animals, Cell Line, Dose-Response Relationship, Immunologic, Immune Tolerance, In Vitro Techniques, Inositol Phosphates metabolism, Lymphocyte Activation, Mice, Protein-Tyrosine Kinases physiology, Receptors, Muscarinic immunology, Second Messenger Systems, Signal Transduction, Time Factors, Type C Phospholipases physiology, CD4-Positive T-Lymphocytes immunology, Receptors, Antigen, T-Cell immunology
Abstract

T cell receptor (TCR)-mediated stimulation of T hybridomas leads to cell activation and lymphokine production that is followed by a long-term hyporesponsiveness. To investigate the biochemical events involved in the induction and maintenance of this antigen receptor hyporesponsiveness or anergy, we have expressed a G protein/PLC beta 1-coupled muscarinic subtype 1 acetylcholine receptor in a murine T cell hybrid. Transfected cells were capable of responding to both muscarinic agonists and TCR ligands by inducing interleukin-2 secretion that was sensitive to cyclosporin A and dexamethasone. Both receptors induced tyrosine kinase (TK) activity, but muscarinic stimulation did not affect tyrosine phosphorylation of PLC gamma 1, nor did the TK inhibitor, herbimycin, block muscarinic receptor-mediated calcium mobilization. These data indicate that in T cells, the muscarinic receptor mediates T cell effector functions by regulating a TK-independent proximal pathway which later converges with the TCR pathway. Using these cells, we have explored the long-term consequences of T cell stimulation via antigen or muscarinic receptors. Our results show that hyporesponsiveness specifically follows TCR engagement and appears to result from a defect in the early signal transduction initiated by TCR cross-linking. A study of TCR-mediated signaling supports this model by showing that tyrosine phosphorylation and calcium mobilization are deficient in hyporesponsive T cells.

Published
1994
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50. Single-chain mono- and bispecific antibody derivatives with novel biological properties and antitumour activity from a COS cell transient expression system.

Author

Hayden MS, Linsley PS, Gayle MA, Bajorath J, Brady WA, Norris NA, Fell HP, Ledbetter JA, and Gilliland LK

Subjects
Amino Acid Sequence, Animals, Antibodies, Monoclonal immunology, Antibody Specificity, Antigens, Neoplasm immunology, Base Sequence, CD3 Complex immunology, Cell Adhesion, Chlorocebus aethiops, DNA Primers chemistry, Genetic Vectors, Humans, Lymphocyte Activation, Molecular Sequence Data, T-Lymphocytes immunology, Antibodies, Bispecific genetics, Antibodies, Monoclonal genetics, Antibodies, Neoplasm immunology, Immunotoxins genetics, Recombinant Fusion Proteins genetics
Abstract

Single-chain antibody molecules were expressed from modified eukaryotic expression vectors as individual protein domains encoded on interchangeable cDNA cassettes. Two different single-chain antibody derivatives were constructed by linking individual light- and heavy-chain variable domains. The first was specific for the L6 tumour-associated antigen and the second was specific for human CD3. Each single-chain variable domain was genetically fused with an Fc 'tag' and expressed as a fusion protein in a COS cell transient transfection system. These single-chain antibody derivatives demonstrated specific binding to cells expressing appropriate antigen and bound with affinities similar to native antibody. The CD3 single chain molecule mediated stronger activation of PLC gamma 1 and similar levels of T-cell proliferation compared with native antibody. A bispecific Fv single-chain cassette was created by fusing the expression cassettes encoding the binding domains for L6 and CD3 single-chain molecules using oligonucleotide primers encoding a short 27-residue 'helical' peptide linker. The CD3-L6 variable domains were fused to the Fc tag and expressed in COS cells. The CD3-L6FvIg bispecific fusion protein mediated adhesion between T cells and L6-positive tumour cells, and stimulated potent T-cell proliferation and cytotoxicity against tumour cells expressing the L6 antigen.

Published
1994

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