Central Pathology Review for Phase III Clinical Trials: The Enabling Effect of Virtual Microscopy

Mróz, Paweł; Parwani, Anil V.; Kulesza, Piotr

doi:10.5858/arpa.2012-0093-ra

Cited by 31 publications

(26 citation statements)

References 28 publications

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“…12 Ab-producing cultures were established of both unmutated (6 of 10) and mutated CLL samples (4 of 10), including two, CLL102 and CLL616, that belonged to previously described stereotypic subsets. 2 Addition of 1.5 μg/ml of the TLR9 ligand CpG-DNA ODN2006 (Invivogen) to CD40L-stimulated cultures resulted in a similar frequency (5/9) of Ab-producing cultures as obtained with R848. Ab concentrations of up to 13 μg/ml were reached, with an average of 4.7 μg/ml (Figure 1c), which are lower than those obtained with R848 stimulation.…”

Section: Conflict Of Interestmentioning

confidence: 91%

“…1 Although widely recognized as an essential measurement of quality assurance and in use for over half a century, only rare reports exist comparing the histopathological evaluation of hematopoietic neoplasms between the central review and the contributing local pathologists in clinical trials. 2,3 The BCR-ABL1-negative myeloproliferative neoplasms (MPNs) primary myelofibrosis (PMF), polycythemia vera (PV) and essential thrombocytopenia (ET) are characterized by variable degrees of bone marrow fibrosis (BMF) at presentation or upon disease progression. [4][5][6] It is well known that development of BMF is an adverse event and has been associated with inferior prognosis in MPN.…”

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confidence: 99%

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The importance of central pathology review in international trials: a comparison of local versus central bone marrow reticulin grading

et al. 2014

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Section: Conflict Of Interestmentioning

confidence: 91%

mentioning

confidence: 99%

The importance of central pathology review in international trials: a comparison of local versus central bone marrow reticulin grading

et al. 2014

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“…By means of WSI platforms and the transfer of digital images together with teleconsultation, it is possible to shorten, simplify and standardise the process of qualification. When considering clinical trials involving large groups of patients, there is also the possibility of standardising quantitative measurement of immunohistochemically-labeled proteins intended as therapeutic targets through applying automated analysis of digital images [55]. This thereby creates huge digital repositories of standardised diagnoses and specimens that can be used for future research on new therapeutic targets.…”

Section: Clinical Trialsmentioning

confidence: 99%

Future perspectives of digital pathology

Prochorec‐Sobieszek

2016

Nowotwory. Journal of Oncology

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Technological advances have enabled innovative solutions to be achieved in pathology based on digital imaging, now superseding those of conventional microscopy. Digital pathology has been defined as 'virtual microscopy' and depends on computer-generated digital imaging of microscope slides (WSI -whole slide imaging) which are in turn created, reviewed, managed, shared, analysed and interpreted. Such WSI systems and digital consulting platforms are now used for teaching, scientific research, telepathology / teleconsultation and diagnostics. They also permit easy and interactive sharing of WSI that can be integrated into other medical information systems. The software for automated image analysis and computer aided diagnosis can thereby make highly accurate diagnoses and help standardise study findings. Despite the technique's many advantages, its noted drawbacks include high equipment and software costs, image quality issues of standardisation and most importantly, that pathologists are reluctant to use it routinely for making diagnoses. NOWOTWORY J Oncol 2016; 66, 4: 277-285

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“…Their use is permitted for consultation (second opinion and frozen section review) and research applications including clinical trials. 1819,20 The use of digital pathology in the clinical setting outside of the USA is governed by local regulation and varies from country to country. The clinical implementation of digital pathology is not cost-neutral, unlike the conversion to digital radiology, and no doubt has slowed its adoption.…”

Section: The Neptune Dpr: New Tools Require New Rulesmentioning

confidence: 99%

Morphology in the Digital Age: Integrating High-Resolution Description of Structural Alterations With Phenotypes and Genotypes

Nast

Lemley

Hodgin

et al. 2015

Seminars in Nephrology

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Conventional light microscopy (CLM) has been used to characterize and classify renal diseases, evaluate histopathology in studies and trials, and educate renal pathologists and nephrologists. The advent of digital pathology, in which a glass slide can be scanned to create whole slide images (WSI) for viewing and manipulating on a computer monitor, provides real and potential advantages over CLM. Software tools such as annotation, morphometry and image analysis can be applied to WSIs for studies or educational purposes, and the digital images are globally available to clinicians, pathologists and investigators. New ways of assessing renal pathology with observational data collection may allow better morphologic correlations and integration with molecular and genetic signatures, refinements of classification schema, and understanding of disease pathogenesis. In multicenter studies, WSI, which require additional quality assurance steps, provide efficiencies by reducing slide shipping and consensus conference costs, and allowing anytime anywhere slide viewing. While validation studies for the routine diagnostic use of digital pathology still are needed, this is a powerful tool currently available for translational research, clinical trials and education in renal pathology.

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Central Pathology Review for Phase III Clinical Trials: The Enabling Effect of Virtual Microscopy

Cited by 31 publications

References 28 publications

The importance of central pathology review in international trials: a comparison of local versus central bone marrow reticulin grading

The importance of central pathology review in international trials: a comparison of local versus central bone marrow reticulin grading

Future perspectives of digital pathology

Morphology in the Digital Age: Integrating High-Resolution Description of Structural Alterations With Phenotypes and Genotypes

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