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Month wise articles
Figures next to the month indicate the number of articles in that month
2021
April
[
4
]
March
[
7
]
February
[
3
]
January
[
6
]
2020
December
[
2
]
November
[
5
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October
[
3
]
September
[
2
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August
[
8
]
July
[
4
]
June
[
2
]
May
[
1
]
April
[
3
]
March
[
3
]
February
[
6
]
January
[
1
]
2019
December
[
6
]
November
[
4
]
September
[
4
]
August
[
3
]
July
[
6
]
June
[
1
]
May
[
2
]
April
[
6
]
March
[
3
]
February
[
4
]
January
[
2
]
2018
December
[
10
]
November
[
4
]
October
[
3
]
September
[
4
]
August
[
1
]
July
[
3
]
June
[
5
]
May
[
4
]
April
[
10
]
March
[
2
]
February
[
4
]
2017
December
[
5
]
November
[
4
]
October
[
3
]
September
[
9
]
July
[
5
]
June
[
2
]
May
[
4
]
April
[
6
]
March
[
6
]
February
[
7
]
2016
December
[
7
]
November
[
5
]
October
[
3
]
September
[
7
]
August
[
1
]
July
[
7
]
May
[
8
]
April
[
7
]
March
[
4
]
February
[
2
]
January
[
5
]
2015
November
[
4
]
October
[
5
]
September
[
5
]
August
[
4
]
July
[
3
]
June
[
19
]
May
[
5
]
April
[
1
]
March
[
5
]
February
[
9
]
January
[
3
]
2014
November
[
2
]
October
[
5
]
September
[
4
]
August
[
6
]
July
[
8
]
June
[
1
]
May
[
3
]
March
[
8
]
February
[
3
]
January
[
4
]
2013
December
[
5
]
November
[
2
]
October
[
4
]
September
[
4
]
August
[
3
]
July
[
3
]
June
[
5
]
May
[
7
]
March
[
18
]
February
[
1
]
January
[
1
]
2012
December
[
6
]
November
[
1
]
October
[
4
]
September
[
4
]
August
[
7
]
July
[
2
]
June
[
1
]
May
[
2
]
April
[
7
]
March
[
6
]
February
[
7
]
January
[
13
]
2011
December
[
3
]
November
[
1
]
October
[
7
]
August
[
9
]
July
[
3
]
June
[
7
]
May
[
3
]
March
[
6
]
February
[
8
]
January
[
6
]
2010
December
[
4
]
November
[
1
]
October
[
6
]
September
[
1
]
August
[
6
]
July
[
6
]
May
[
5
]
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Original Article:
Computer-assisted imaging algorithms facilitate histomorphometric quantification of kidney damage in rodent renal failure models
Marcin Klapczynski, Gerard D Gagne, Sherry J Morgan, Kelly J Larson, Bruce E LeRoy, Eric A Blomme, Bryan F Cox, Eugene W Shek
J Pathol Inform
2012, 3:20 (28 April 2012)
DOI
:10.4103/2153-3539.95456
PMID
:22616032
Introduction:
Surgical 5/6 nephrectomy and adenine-induced kidney failure in rats are frequently used models of progressive renal failure. In both models, rats develop significant morphological changes in the kidneys and quantification of these changes can be used to measure the efficacy of prophylactic or therapeutic approaches. In this study, the Aperio Genie Pattern Recognition technology, along with the Positive Pixel Count, Nuclear and Rare Event algorithms were used to quantify histological changes in both rat renal failure models.
Methods:
Analysis was performed on digitized slides of whole kidney sagittal sections stained with either hematoxylin and eosin or immunohistochemistry with an anti-nestin antibody to identify glomeruli, regenerating tubular epithelium, and tubulointerstitial myofibroblasts. An anti-polymorphonuclear neutrophil (PMN) antibody was also used to investigate neutrophil tissue infiltration.
Results:
Image analysis allowed for rapid and accurate quantification of relevant histopathologic changes such as increased cellularity and expansion of glomeruli, renal tubular dilatation, and degeneration, tissue inflammation, and mineral aggregation. The algorithms provided reliable and consistent results in both control and experimental groups and presented a quantifiable degree of damage associated with each model.
Conclusion:
These algorithms represent useful tools for the uniform and reproducible characterization of common histomorphologic features of renal injury in rats.
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Research Article:
Estrogen receptor testing and 10-year mortality from breast cancer: A model for determining testing strategy
Christopher Naugler
J Pathol Inform
2012, 3:19 (28 April 2012)
DOI
:10.4103/2153-3539.95452
PMID
:22616031
Background:
The use of adjuvant tamoxifen therapy in the treatment of estrogen receptor (ER) expressing breast carcinomas represents a major advance in personalized cancer treatment. Because there is no benefit (and indeed there is increased morbidity and mortality) associated with the use of tamoxifen therapy in ER-negative breast cancer, its use is restricted to women with ER expressing cancers. However, correctly classifying cancers as ER positive or negative has been challenging given the high reported false negative test rates for ER expression in surgical specimens. In this paper I model practice recommendations using published information from clinical trials to address the question of whether there is a false negative test rate above which it is more efficacious to forgo ER testing and instead treat all patients with tamoxifen regardless of ER test results.
Methods:
I used data from randomized clinical trials to model two different hypothetical treatment strategies: (1) the current strategy of treating only ER positive women with tamoxifen and (2) an alternative strategy where all women are treated with tamoxifen regardless of ER test results. The variables used in the model are literature-derived survival rates of the different combinations of ER positivity and treatment with tamoxifen, varying true ER positivity rates and varying false negative ER testing rates. The outcome variable was hypothetical 10-year survival.
Results:
The model predicted that there will be a range of true ER rates and false negative test rates above which it would be more efficacious to treat all women with breast cancer with tamoxifen and forgo ER testing. This situation occurred with high true positive ER rates and false negative ER test rates in the range of 20-30%.
Conclusions:
It is hoped that this model will provide an example of the potential importance of diagnostic error on clinical outcomes and furthermore will give an example of how the effect of that error could be modeled using real-world data from clinical trials.
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Technical note:
Investigation into diagnostic agreement using automated computer-assisted histopathology pattern recognition image analysis
Joshua D Webster, Aleksandra M Michalowski, Jennifer E Dwyer, Kara N Corps, Bih-Rong Wei, Tarja Juopperi, Shelley B Hoover, R Mark Simpson
J Pathol Inform
2012, 3:18 (18 April 2012)
DOI
:10.4103/2153-3539.95130
PMID
:22616030
The extent to which histopathology pattern recognition image analysis (PRIA) agrees with microscopic assessment has not been established. Thus, a commercial PRIA platform was evaluated in two applications using whole-slide images. Substantial agreement, lacking significant constant or proportional errors, between PRIA and manual morphometric image segmentation was obtained for pulmonary metastatic cancer areas (Passing/Bablok regression). Bland-Altman analysis indicated heteroscedastic measurements and tendency toward increasing variance with increasing tumor burden, but no significant trend in mean bias. The average between-methods percent tumor content difference was -0.64. Analysis of between-methods measurement differences relative to the percent tumor magnitude revealed that method disagreement had an impact primarily in the smallest measurements (tumor burden <3%). Regression-based 95% limits of agreement indicated substantial agreement for method interchangeability. Repeated measures revealed concordance correlation of >0.988, indicating high reproducibility for both methods, yet PRIA reproducibility was superior (C.V.: PRIA = 7.4, manual = 17.1). Evaluation of PRIA on morphologically complex teratomas led to diagnostic agreement with pathologist assessments of pluripotency on subsets of teratomas. Accommodation of the diversity of teratoma histologic features frequently resulted in detrimental trade-offs, increasing PRIA error elsewhere in images. PRIA error was nonrandom and influenced by variations in histomorphology. File-size limitations encountered while training algorithms and consequences of spectral image processing dominance contributed to diagnostic inaccuracies experienced for some teratomas. PRIA appeared better suited for tissues with limited phenotypic diversity. Technical improvements may enhance diagnostic agreement, and consistent pathologist input will benefit further development and application of PRIA.
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Research Article:
Compressing pathology whole-slide images using a human and model observer evaluation
Elizabeth A Krupinski, Jeffrey P Johnson, Stacey Jaw, Anna R Graham, Ronald S Weinstein
J Pathol Inform
2012, 3:17 (18 April 2012)
DOI
:10.4103/2153-3539.95129
PMID
:22616029
Introduction:
We aim to determine to what degree whole-slide images (WSI) can be compressed without impacting the ability of the pathologist to distinguish benign from malignant tissues. An underlying goal is to demonstrate the utility of a visual discrimination model (VDM) for predicting observer performance.
Materials and Methods:
A total of 100 regions of interest (ROIs) from a breast biopsy whole-slide images at five levels of JPEG 2000 compression (8:1, 16:1, 32:1, 64:1, and 128:1) plus the uncompressed version were shown to six pathologists to determine benign versus malignant status.
Results:
There was a significant decrease in performance as a function of compression ratio (F = 14.58,
P
< 0.0001). The visibility of compression artifacts in the test images was predicted using a VDM. Just-noticeable difference (JND) metrics were computed for each image, including the mean, median, ≥90th percentiles, and maximum values. For comparison, PSNR (peak signal-to-noise ratio) and Structural Similarity (SSIM) were also computed. Image distortion metrics were computed as a function of compression ratio and averaged across test images. All of the JND metrics were found to be highly correlated and differed primarily in magnitude. Both PSNR and SSIM decreased with bit rate, correctly reflecting a loss of image fidelity with increasing compression. Observer performance as measured by the Receiver Operating Characteristic area under the curve (ROC Az) was nearly constant up to a compression ratio of 32:1, then decreased significantly for 64:1 and 128:1 compression levels. The initial decline in Az occurred around a mean JND of 3, Minkowski JND of 4, and 99th percentile JND of 6.5.
Conclusion:
Whole-slide images may be compressible to relatively high levels before impacting WSI interpretation performance. The VDM metrics correlated well with artifact conspicuity and human performance.
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Research Article:
Changes, disruption and innovation: An investigation of the introduction of new health information technology in a microbiology laboratory
George Toouli, Andrew Georgiou, Johanna Westbrook
J Pathol Inform
2012, 3:16 (18 April 2012)
DOI
:10.4103/2153-3539.95128
PMID
:22616028
Background:
It is expected that health information technology (HIT) will deliver a safer, more efficient and effective health care system. The aim of this study was to undertake a qualitative and video-ethnographic examination of the impact of information technologies on work processes in the reception area of a Microbiology Department, to ascertain what changed, how it changed and the impact of the change.
Materials and Methods:
The setting for this study was the microbiology laboratory of a large tertiary hospital in Sydney. The study consisted of qualitative (interview and focus group) data and observation sessions for the period August 2005 to October 2006 along with video footage shot in three sessions covering the original system and the two stages of the Cerner implementation. Data analysis was assisted by NVivo software and process maps were produced from the video footage.
Results:
There were two laboratory information systems observed in the video footage with computerized provider order entry introduced four months later. Process maps highlighted the large number of pre data entry steps with the original system whilst the newer system incorporated many of these steps in to the data entry stage. However, any time saved with the new system was offset by the requirement to complete some data entry of patient information not previously required. Other changes noted included the change of responsibilities for the reception staff and the physical changes required to accommodate the increased activity around the data entry area.
Conclusions:
Implementing a new HIT is always an exciting time for any environment but ensuring that the implementation goes smoothly and with minimal trouble requires the administrator and their team to plan well in advance for staff training, physical layout and possible staff resource reallocation.
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Review Article:
Handheld computing in pathology
Seung Park, Anil Parwani, Mahadev Satyanarayanan, Liron Pantanowitz
J Pathol Inform
2012, 3:15 (18 April 2012)
DOI
:10.4103/2153-3539.95127
PMID
:22616027
Handheld computing has had many applications in medicine, but relatively few in pathology. Most reported uses of handhelds in pathology have been limited to experimental endeavors in telemedicine or education. With recent advances in handheld hardware and software, along with concurrent advances in whole-slide imaging (WSI), new opportunities and challenges have presented themselves. This review addresses the current state of handheld hardware and software, provides a history of handheld devices in medicine focusing on pathology, and presents future use cases for such handhelds in pathology.
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Commentary:
Comment on "Quality evaluation of microscopy and scanned histological images for diagnostic purposes": Are scanners better than microscopes?
Yukako Yagi, Liron Pantanowitz
J Pathol Inform
2012, 3:14 (18 April 2012)
PMID
:22616026
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