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jhc.2024.v8.i2.1


Editorial

DOI: https://www.doi.org/10.69950/jhc.2024.v8.i2.1

 Reporting Renal Biopsies with Limited Resources

*Banu SG

Reporting renal biopsies needs multiple specialized techniques to aid histopathology. Though histopathology correlating clinical features can provisionally diagnose a number of renal parenchymal disorders, some of those diagnoses lack confirmation, while some others remain incomplete. In many developing countries like ours, renal biopsies are usually reported with history, clinical features, histopathology and direct immunofluorescence (DIF) study. Although this practice can diagnose diseases like minimal change disease, infection associated glomerulonephritis, diabetic nephropathy, membranous nephropathy and IgA nephropathy with variable confidence, many diagnoses need electron microscopy, immunohistochemistry and molecular study for their confirmation. Concerns arise as some important medical approaches namely ‘treatment of disease’, ‘prediction of prognosis’ and ‘research’ are based on these diagnoses. Incomplete diagnosis can badly affect patient management and research authenticity.
Focal segmental glomerulosclerosis (FSGS) denotes a common renal disorder. But more importantly, it implies a histomorphological pattern seen in many renal biopsies having other disorders that are progressing to chronicity. While the latter disorders can be diagnosed with the help of DIF study (when they are immune-mediated), the true FSGS, which is basically a podocytopathy, needs electron microscopy to see the podocyte foot process effacement, podocyte loss and hypertrophy. Diseases with organoid deposits like amyloidosis, fibrillary glomerulonephritis, immunoglobulin/light chain deposition disease and others need special stains, immunohistochemistry and electron microscopy for confirmation of their diagnosis. Molecular study is needed in many cases to detect genetic alterations. Newer ancillary techniques including image analysis and AI-based computational approach have already moved into the diagnostic panel of renal biopsies in the developed countries. In this modern era, with a huge load of kidney patients in our country, we are remaining satisfied with diagnosis of some common diseases using the oldest tools, as if less common diseases do not occur in our people. This attitude of ours should be changed. More pathologists should be trained in reporting renal biopsies, and they must have modern laboratory facilities to make proper diagnoses of the renal diseases. Bigger institutions should come forward with offers of logistic support.
*Dr. Sultana Gulshana Banu, Professor, Department of Pathology, BSMMU, Shahbag, Dhaka. sgb.bsmmu@gmail.com

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Original Contribution

 Evaluation of Immunohistochemical Expression of p53 in Colorectal Carcinoma

 *Mouri MJ,1 Kabir E,2 Begum S3

 Abstract

Background: The most common gastrointestinal malignancy is colorectal carcinoma and is a major cause of morbidity and mortality. In colorectal carcinoma the most frequently mutated gene is p53 tumor suppressor gene. Mutation of p53 gene gives rise to abnormal protein which can be easily detected by immunohistochemistry. Expression of mutant p53 protein has been associated with poor clinical outcome and increased risk of death due to increased aggressiveness of the disease.

ObjectiveThe aim of the study was to see the clinicopathological correlation of mutant p53 expression in colorectal carcinoma.

Method Total 50 paraffin embedded tissue blocks of histopathologically diagnosed cases of colorectal cancer were evaluated by immunohistochemical staining for mutant p53 expression. The study was performed in Sir Salimullah Medical College, Dhaka (from March, 2018 to February, 2020).

Results: Out of 50 patients studied, 29 cases (58%) expressed mutant p53 protein in the nucleus of malignant cells. There was significant association between  p53  protein expression and clinicopathologic variables such as age (<40 years vs >40 years, p=0.032), site of tumor (left vs right colon, p=0.028), pathological type (mucinous vs non mucinous, p=0.039), grade (a greater tendency towards poor differentiation, p= 0.039), advanced stage (both TNM and Dukes), whereas no significant association was found between mutant p53 protien expression and other parameters like gender and morphological types.

Conclusion: The results of this current study revealed that mutant p53 positive colorectal cancer tended to be related to a higher grade of malignancy, advanced tumor stage and mucinous morphology. The results of this current study revealed that mutant p53 positive colorectal cancer tended to be related to a higher grade of malignancy, advanced tumor stage and mucinous morphology. So, p53 is an important immunohistochemical marker for colorectal cancer patients

 

[Journal of Histopathology and Cytopathology, 2024 Jan; 8 (1):10-18]

 

Keywords: Colorectal cancer, p53, Immunohistochemistry

 

  1. *Dr. Mahfuza Jebun  Mouri; Lecturer, Department of Pathology, Shaheed Suhrawardy Medical College, Sher-E-Bangla Nagar, Dhaka.  mouri@gmail.com.
  2. Enamul Kabir, Professor, Department of Pathology, Popular Medical College, Dhaka.
  3. Shahnaj Begum, Professor, Department of Pathology, Sir Salimullah Medical College, Dhaka.

 

*For correspondence

Introduction

Colorectal cancer (CRC) is the most common malignancy of gastrointestinal tract and it is one of the leading causes of cancer related morbidity and mortality in the world. Over 1.9 million new CRC cases and 930 000 deaths were estimated in 2020 and the burden of CRC is projected to increase to 3.2 million new cases and 1.6 million deaths by 2040.1 Adenocarcinoma is the most common form of colorectal cancer (>95%).2 The essential elements of the pathological assessment of colorectal cancer resection specimens include the pathologic determination of TNM stage, tumor type, histologic grade, status of resection margins, and vascular invasion.3 ……

 

Methods

This cross sectional study was conducted in Department of Pathology, Sir Salimullah Medical College, Dhaka during the period from March 2018 to February, 2020. …………..

 

Results

The age range of study population was from 32 to 75 years and more than one third (42.0%) of patients belonged to age 50-59 years. Among the patients 64% were male. ……….

 

Table I: Distribution of the study cases by P53 Expression (n=50)

P53 Expression Number of cases Percentage (%) of cases
<5% (Negative) 21 42.0
5-25% (Weakly positive) 11 22.0
26-75% (Moderately positive) 9 18.0
>75% (Strongly positive) 9 18.0

Figure 1. Photomicrograph showing H & E stained section well differentiated adenocarcinoma of colon

 

Discussion

Many studies reveal that the mutant p53 immunostain is very high in CRC. The positivity rate is reported being between 43% and 86.36%.14,15,16  In the present study, out of 50 cases of colorectal carcinoma samples, 29 cases (58%) displayed mutant p53 protein overexpression. ………

 

References

  1. Morgan E, Arnold M, Gini A, Lorenzoni V, Cabasag CJ, Laversanne M, Vignat J, Ferlay J, Murphy N, Bray F. Global burden of colorectal cancer in 2020 and 2040: Incidence and mortality estimates from GLOBOCAN. Gut. 2023 Feb 1; 72(2):338-44.
  2. Thrumurthy SG, Thrumurthy SS, Gilbert CE, Ross P, Haji A. Colorectal adenocarcinoma: risks, prevention and diagnosis. Bmj. 2016 Jul 14; 354.
  3. Compton CC. Colorectal carcinoma: diagnostic, prognostic, and molecular features. Modern Pathology. 2003 Apr 1; 16(4):376-88…….

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