JCDR - Breast neoplasms, Immunohistochemisty, Stromal cells

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Dr Mohan Z Mani

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I wish all success to your journal and look forward to sending you any suitable similar article in future"

Dr Mohan Z Mani,
Professor & Head,
Department of Dermatolgy,
Believers Church Medical College,
Thiruvalla, Kerala
On Sep 2018

Prof. Somashekhar Nimbalkar

"Over the last few years, we have published our research regularly in Journal of Clinical and Diagnostic Research. Having published in more than 20 high impact journals over the last five years including several high impact ones and reviewing articles for even more journals across my fields of interest, we value our published work in JCDR for their high standards in publishing scientific articles. The ease of submission, the rapid reviews in under a month, the high quality of their reviewers and keen attention to the final process of proofs and publication, ensure that there are no mistakes in the final article. We have been asked clarifications on several occasions and have been happy to provide them and it exemplifies the commitment to quality of the team at JCDR."

Prof. Somashekhar Nimbalkar
Head, Department of Pediatrics, Pramukhswami Medical College, Karamsad
Chairman, Research Group, Charutar Arogya Mandal, Karamsad
National Joint Coordinator - Advanced IAP NNF NRP Program
Ex-Member, Governing Body, National Neonatology Forum, New Delhi
Ex-President - National Neonatology Forum Gujarat State Chapter
Department of Pediatrics, Pramukhswami Medical College, Karamsad, Anand, Gujarat.
On Sep 2018

Dr. Kalyani R

"Journal of Clinical and Diagnostic Research is at present a well-known Indian originated scientific journal which started with a humble beginning. I have been associated with this journal since many years. I appreciate the Editor, Dr. Hemant Jain, for his constant effort in bringing up this journal to the present status right from the scratch. The journal is multidisciplinary. It encourages in publishing the scientific articles from postgraduates and also the beginners who start their career. At the same time the journal also caters for the high quality articles from specialty and super-specialty researchers. Hence it provides a platform for the scientist and researchers to publish. The other aspect of it is, the readers get the information regarding the most recent developments in science which can be used for teaching, research, treating patients and to some extent take preventive measures against certain diseases. The journal is contributing immensely to the society at national and international level."

Dr Kalyani R
Professor and Head
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Sri Devaraj Urs Medical College
Sri Devaraj Urs Academy of Higher Education and Research , Kolar, Karnataka
On Sep 2018

Dr. Saumya Navit

"As a peer-reviewed journal, the Journal of Clinical and Diagnostic Research provides an opportunity to researchers, scientists and budding professionals to explore the developments in the field of medicine and dentistry and their varied specialities, thus extending our view on biological diversities of living species in relation to medicine.
‘Knowledge is treasure of a wise man.’ The free access of this journal provides an immense scope of learning for the both the old and the young in field of medicine and dentistry as well. The multidisciplinary nature of the journal makes it a better platform to absorb all that is being researched and developed. The publication process is systematic and professional. Online submission, publication and peer reviewing makes it a user-friendly journal.
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I wish JCDR a great success and I hope that journal will soar higher with the passing time."

Dr Saumya Navit
Professor and Head
Department of Pediatric Dentistry
Saraswati Dental College
Lucknow
On Sep 2018

Dr. Arunava Biswas

"My sincere attachment with JCDR as an author as well as reviewer is a learning experience . Their systematic approach in publication of article in various categories is really praiseworthy.
Their prompt and timely response to review's query and the manner in which they have set the reviewing process helps in extracting the best possible scientific writings for publication.
It's a honour and pride to be a part of the JCDR team. My very best wishes to JCDR and hope it will sparkle up above the sky as a high indexed journal in near future."

Dr. Arunava Biswas
MD, DM (Clinical Pharmacology)
Assistant Professor
Department of Pharmacology
Calcutta National Medical College & Hospital , Kolkata

Dr. C.S. Ramesh Babu
" Journal of Clinical and Diagnostic Research (JCDR) is a multi-specialty medical and dental journal publishing high quality research articles in almost all branches of medicine. The quality of printing of figures and tables is excellent and comparable to any International journal. An added advantage is nominal publication charges and monthly issue of the journal and more chances of an article being accepted for publication. Moreover being a multi-specialty journal an article concerning a particular specialty has a wider reach of readers of other related specialties also. As an author and reviewer for several years I find this Journal most suitable and highly recommend this Journal."
Best regards,
C.S. Ramesh Babu,
Associate Professor of Anatomy,
Muzaffarnagar Medical College,
Muzaffarnagar.
On Aug 2018

Dr. Arundhathi. S
"Journal of Clinical and Diagnostic Research (JCDR) is a reputed peer reviewed journal and is constantly involved in publishing high quality research articles related to medicine. Its been a great pleasure to be associated with this esteemed journal as a reviewer and as an author for a couple of years. The editorial board consists of many dedicated and reputed experts as its members and they are doing an appreciable work in guiding budding researchers. JCDR is doing a commendable job in scientific research by promoting excellent quality research & review articles and case reports & series. The reviewers provide appropriate suggestions that improve the quality of articles. I strongly recommend my fraternity to encourage JCDR by contributing their valuable research work in this widely accepted, user friendly journal. I hope my collaboration with JCDR will continue for a long time".

Dr. Arundhathi. S
MBBS, MD (Pathology),
Sanjay Gandhi institute of trauma and orthopedics,
Bengaluru.
On Aug 2018

Dr. Mamta Gupta,
"It gives me great pleasure to be associated with JCDR, since last 2-3 years. Since then I have authored, co-authored and reviewed about 25 articles in JCDR. I thank JCDR for giving me an opportunity to improve my own skills as an author and a reviewer.
It 's a multispecialty journal, publishing high quality articles. It gives a platform to the authors to publish their research work which can be available for everyone across the globe to read. The best thing about JCDR is that the full articles of all medical specialties are available as pdf/html for reading free of cost or without institutional subscription, which is not there for other journals. For those who have problem in writing manuscript or do statistical work, JCDR comes for their rescue.
The journal has a monthly publication and the articles are published quite fast. In time compared to other journals. The on-line first publication is also a great advantage and facility to review one's own articles before going to print. The response to any query and permission if required, is quite fast; this is quite commendable. I have a very good experience about seeking quick permission for quoting a photograph (Fig.) from a JCDR article for my chapter authored in an E book. I never thought it would be so easy. No hassles.
Reviewing articles is no less a pain staking process and requires in depth perception, knowledge about the topic for review. It requires time and concentration, yet I enjoy doing it. The JCDR website especially for the reviewers is quite user friendly. My suggestions for improving the journal is, more strict review process, so that only high quality articles are published. I find a a good number of articles in Obst. Gynae, hence, a new journal for this specialty titled JCDR-OG can be started. May be a bimonthly or quarterly publication to begin with. Only selected articles should find a place in it.
An yearly reward for the best article authored can also incentivize the authors. Though the process of finding the best article will be not be very easy. I do not know how reviewing process can be improved. If an article is being reviewed by two reviewers, then opinion of one can be communicated to the other or the final opinion of the editor can be communicated to the reviewer if requested for. This will help one’s reviewing skills.
My best wishes to Dr. Hemant Jain and all the editorial staff of JCDR for their untiring efforts to bring out this journal. I strongly recommend medical fraternity to publish their valuable research work in this esteemed journal, JCDR".

Dr. Mamta Gupta
Consultant
(Ex HOD Obs &Gynae, Hindu Rao Hospital and associated NDMC Medical College, Delhi)
Aug 2018

Dr. Rajendra Kumar Ghritlaharey

"I wish to thank Dr. Hemant Jain, Editor-in-Chief Journal of Clinical and Diagnostic Research (JCDR), for asking me to write up few words.
Writing is the representation of language in a textual medium i e; into the words and sentences on paper. Quality medical manuscript writing in particular, demands not only a high-quality research, but also requires accurate and concise communication of findings and conclusions, with adherence to particular journal guidelines. In medical field whether working in teaching, private, or in corporate institution, everyone wants to excel in his / her own field and get recognised by making manuscripts publication.

Authors are the souls of any journal, and deserve much respect. To publish a journal manuscripts are needed from authors. Authors have a great responsibility for producing facts of their work in terms of number and results truthfully and an individual honesty is expected from authors in this regards. Both ways its true "No authors-No manuscripts-No journals" and "No journals–No manuscripts–No authors". Reviewing a manuscript is also a very responsible and important task of any peer-reviewed journal and to be taken seriously. It needs knowledge on the subject, sincerity, honesty and determination. Although the process of reviewing a manuscript is a time consuming task butit is expected to give one's best remarks within the time frame of the journal.
Salient features of the JCDR: It is a biomedical, multidisciplinary (including all medical and dental specialities), e-journal, with wide scope and extensive author support. At the same time, a free text of manuscript is available in HTML and PDF format. There is fast growing authorship and readership with JCDR as this can be judged by the number of articles published in it i e; in Feb 2007 of its first issue, it contained 5 articles only, and now in its recent volume published in April 2011, it contained 67 manuscripts. This e-journal is fulfilling the commitments and objectives sincerely, (as stated by Editor-in-chief in his preface to first edition) i e; to encourage physicians through the internet, especially from the developing countries who witness a spectrum of disease and acquire a wealth of knowledge to publish their experiences to benefit the medical community in patients care. I also feel that many of us have work of substance, newer ideas, adequate clinical materials but poor in medical writing and hesitation to submit the work and need help. JCDR provides authors help in this regards.
Timely publication of journal: Publication of manuscripts and bringing out the issue in time is one of the positive aspects of JCDR and is possible with strong support team in terms of peer reviewers, proof reading, language check, computer operators, etc. This is one of the great reasons for authors to submit their work with JCDR. Another best part of JCDR is "Online first Publications" facilities available for the authors. This facility not only provides the prompt publications of the manuscripts but at the same time also early availability of the manuscripts for the readers.
Indexation and online availability: Indexation transforms the journal in some sense from its local ownership to the worldwide professional community and to the public.JCDR is indexed with Embase & EMbiology, Google Scholar, Index Copernicus, Chemical Abstracts Service, Journal seek Database, Indian Science Abstracts, to name few of them. Manuscriptspublished in JCDR are available on major search engines ie; google, yahoo, msn.
In the era of fast growing newer technologies, and in computer and internet friendly environment the manuscripts preparation, submission, review, revision, etc and all can be done and checked with a click from all corer of the world, at any time. Of course there is always a scope for improvement in every field and none is perfect. To progress, one needs to identify the areas of one's weakness and to strengthen them.
It is well said that "happy beginning is half done" and it fits perfectly with JCDR. It has grown considerably and I feel it has already grown up from its infancy to adolescence, achieving the status of standard online e-journal form Indian continent since its inception in Feb 2007. This had been made possible due to the efforts and the hard work put in it. The way the JCDR is improving with every new volume, with good quality original manuscripts, makes it a quality journal for readers. I must thank and congratulate Dr Hemant Jain, Editor-in-Chief JCDR and his team for their sincere efforts, dedication, and determination for making JCDR a fast growing journal.
Every one of us: authors, reviewers, editors, and publisher are responsible for enhancing the stature of the journal. I wish for a great success for JCDR."

Thanking you
With sincere regards
Dr. Rajendra Kumar Ghritlaharey, M.S., M. Ch., FAIS
Associate Professor,
Department of Paediatric Surgery, Gandhi Medical College & Associated
Kamla Nehru & Hamidia Hospitals Bhopal, Madhya Pradesh 462 001 (India)
E-mail: drrajendrak1@rediffmail.com
On May 11,2011

Dr. Shankar P.R.

"On looking back through my Gmail archives after being requested by the journal to write a short editorial about my experiences of publishing with the Journal of Clinical and Diagnostic Research (JCDR), I came across an e-mail from Dr. Hemant Jain, Editor, in March 2007, which introduced the new electronic journal. The main features of the journal which were outlined in the e-mail were extensive author support, cash rewards, the peer review process, and other salient features of the journal.
Over a span of over four years, we (I and my colleagues) have published around 25 articles in the journal. In this editorial, I plan to briefly discuss my experiences of publishing with JCDR and the strengths of the journal and to finally address the areas for improvement.
My experiences of publishing with JCDR: Overall, my experiences of publishing withJCDR have been positive. The best point about the journal is that it responds to queries from the author. This may seem to be simple and not too much to ask for, but unfortunately, many journals in the subcontinent and from many developing countries do not respond or they respond with a long delay to the queries from the authors 1. The reasons could be many, including lack of optimal secretarial and other support. Another problem with many journals is the slowness of the review process. Editorial processing and peer review can take anywhere between a year to two years with some journals. Also, some journals do not keep the contributors informed about the progress of the review process. Due to the long review process, the articles can lose their relevance and topicality. A major benefit with JCDR is the timeliness and promptness of its response. In Dr Jain's e-mail which was sent to me in 2007, before the introduction of the Pre-publishing system, he had stated that he had received my submission and that he would get back to me within seven days and he did!
Most of the manuscripts are published within 3 to 4 months of their submission if they are found to be suitable after the review process. JCDR is published bimonthly and the accepted articles were usually published in the next issue. Recently, due to the increased volume of the submissions, the review process has become slower and it ?? Section can take from 4 to 6 months for the articles to be reviewed. The journal has an extensive author support system and it has recently introduced a paid expedited review process. The journal also mentions the average time for processing the manuscript under different submission systems - regular submission and expedited review.
Strengths of the journal: The journal has an online first facility in which the accepted manuscripts may be published on the website before being included in a regular issue of the journal. This cuts down the time between their acceptance and the publication. The journal is indexed in many databases, though not in PubMed. The editorial board should now take steps to index the journal in PubMed. The journal has a system of notifying readers through e-mail when a new issue is released. Also, the articles are available in both the HTML and the PDF formats. I especially like the new and colorful page format of the journal. Also, the access statistics of the articles are available. The prepublication and the manuscript tracking system are also helpful for the authors.
Areas for improvement: In certain cases, I felt that the peer review process of the manuscripts was not up to international standards and that it should be strengthened. Also, the number of manuscripts in an issue is high and it may be difficult for readers to go through all of them. The journal can consider tightening of the peer review process and increasing the quality standards for the acceptance of the manuscripts. I faced occasional problems with the online manuscript submission (Pre-publishing) system, which have to be addressed.
Overall, the publishing process with JCDR has been smooth, quick and relatively hassle free and I can recommend other authors to consider the journal as an outlet for their work."

Dr. P. Ravi Shankar
KIST Medical College, P.O. Box 14142, Kathmandu, Nepal.
E-mail: ravi.dr.shankar@gmail.com
On April 2011 Anuradha

Dear team JCDR, I would like to thank you for the very professional and polite service provided by everyone at JCDR. While i have been in the field of writing and editing for sometime, this has been my first attempt in publishing a scientific paper.Thank you for hand-holding me through the process.

Dr. Anuradha
E-mail: anuradha2nittur@gmail.com
On Jan 2020

Important Notice

Original article / research

Year : 2022 | Month : April | Volume : 16 | Issue : 4 | Page : EC36 - EC40

Full Version

Clinicopathological Study of Breast Lesions with Special Reference to the Role of CD34 Immunostaining in Diagnosis- A Cross-sectional Study from a Tertiary Care Hospital of West Bengal, India

Published: April 1, 2022 | DOI: https://doi.org/10.7860/JCDR/2022/55414.16241
Ambika Prasad Chakraborty, Debasis Mukhopadhyay, Arnab Mandal, Aparajita Samaddar, Swapan Pathak

1. Postgraduate Trainee, Department of Pathology, Bankura Sammilani Medical College, Bankura, West Bengal, India. 2. Associate Professor, Department of Pathology, Bankura Sammilani Medical College, Bankura, West Bengal, India. 3. Associate Professor, Department of General Surgery, Bankura Sammilani Medical College, Bankura, West Bengal, India. 4. Assistant Professor, Department of Pathology, Medical College and Hospital, Kolkata, West Bengal, India. 5. Professor, Department of Pathology, Bankura Sammilani Medical College, Bankura, West Bengal, India.

Correspondence Address :
Dr. Aparajita Samaddar,
4/3K/297, Ho Chi Minh Sarani, Sakuntala Park, Kolkata-700061, West Bengal, India.
E-mail: aparajita.samaddar@gmail.com

Abstract

Introduction: Breast carcinoma is the most common cancer among women and leading cause of mortality. Prognosis of breast carcinoma primarily depends on early detection. The changes in molecular and antigenic expression in stromal micro-environment surrounding the tumour cells was noted earlier in tumours of skin and gastrointestinal tract which showed loss of Cluster of Differentiation 34 (CD34) expression in stromal cell of malignant tumours.

Aim: To evaluate the intensity of CD34 staining in benign, borderline and malignant lesions of breast and to find out whether it can help to differentiate benign and malignant lesions from borderline and in-situ carcinomas.

Materials and Methods: This was a cross-sectional prospective study done over a period of 18 months in a tertiary care hospital of Bankura, West Bengal, India. Total 78 specimens of breast lesions obtained by lumpectomy and Modified Radical Mastectomy (MRM) were first evaluated on routine histology and classified as benign, borderline or malignant accordingly. Subsequent immunohistochemical staining was performed for CD34 and intensity of expression in stromal cells was graded from 0 to 3+. Then comparison of CD34 expression in different lesions was done and level of significance was assessed by using Student’s t-test.

Results: Out of total 78 cases evaluated, 50 (64.1%) were categorised as benign and rest 28 (35.9%) were either premalignant or malignant lesions. Intensity of CD34 expression was found to be significantly higher in benign and in-situ lesions compared to malignant epithelial lesions of breast (p<0.05) whereas those between borderline and malignant phyllodes found to be statistically non significant (p-value 0.342).

Conclusion: CD34 immunostaining can help to differentiate benign and in-situ carcinomas from invasive carcinomas, however, its role in differentiating borderline from malignant phyllodes tumour is limited.

Keywords

Breast neoplasms, Immunohistochemisty, Stromal cells

Breast lesions are extremely heterogenous in nature encompassing wide range of benign, borderline and malignant tumours. Breast carcinoma is the second most common cause of cancer death only after lung carcinoma (1). Though histopathology is considered as gold standard for diagnosis of breast lesions, but immunohistochemical study also plays a crucial role where histological diagnosis is inconclusive especially in differentiating invasive carcinomas from in-situ carcinomas. The growth, differentiation and invasiveness of the breast tumour is tightly regulated by stromal cells including fibroblasts, myoepithelial cells and leukocytes (2). Normal mammary stroma strongly expresses CD34 in most of the fibrocytes (3). CD34 is a transmembrane glycoprotein involved in regulation of cell adhesion and signal transduction (4). It is found in mesenchymal cells of other organs also like prostate, urinary bladder, fallopian tube, thyroid gland, pancreas, colon, uterine cervix and testis (5).

Malignancies arising in aforesaid organs showed loss of CD34 expression and gain of alpha Smooth Muscle Actin (α-SMA) positive myofibroblasts indicating the role of this change in antigenic expression in pathogenesis of tumour progression (4),(6). Similarly in breast carcinoma CD34 positive fibrocytes undergo alteration in morphology and antigenic expression. They acquire plump myofibroblast like appearance and show loss of CD34 expression and acquisition of α-SMA (7). This is known as myofibroblastic differentiation. It has been suggested that there is an inverse relationship between CD34 expression and myofibroblastic differentiation (8). Only limited numbers of literatures are available till date to evaluate the diagnostic value of CD34 expression in breast tumours which necessitates further study. With better understanding of changes in stromal micro-environment, this study may help in developing newer target therapy in future. Previous studies did not correlate CD34 expression with clinical staging of breast cancer.

Material and Methods

The present study was conducted to evaluate the intensity of CD34 expression in benign, borderline and malignant lesions of breast and also to find out whether it can help to differentiate borderline and in-situ lesions from benign and malignant neoplasms as there is often diagnostic dilemma, experienced on routine histopathology. An attempt was also made to find out the relation between intensity of CD34 staining and clinical stage of malignant breast tumours.

Inclusion criteria: All the lumpectomy and mastectomy specimens of breast lesions obtained from patients aged ≥18 years presented to the General Surgery Outpatient Department (OPD) with breast lump submitted in properly labeled 10% formalin filled container to the Department of Pathology during the study period with duly filled in histopathology requisition form containing details of patient’s age, sex, side of lesion were included in the present study.

Exclusion criteria: The specimens of known inflammatory conditions, infectious diseases or specimens sent without formalin were excluded from the present study.

Sample size calculation: Sample size was calculated by applying the formula 4pq/e2; where ‘p’ is the prevalence. The prevalence of CD34 positivity in stromal cell of high grade DCIS was taken as 12% (9). So, p=0.12; q=(1-p) and e=allowable error (8% in the present study)=0.08. Thus, the final sample size (n) calculated was 64. To avoid bias, a total of 78 cases of lumpectomy and mastectomy specimens of breast were included in the present study.

Study Procedure

Total 78 cases of lumpectomy and mastectomy specimens of breast were included in the present study. After receiving the sample gross inspection was done and the size and appearance of the tumour, number of lymph nodes etc., were recorded. The sections from the representative areas were submitted for further processing. All the sections were stained by routine Haematoxylin and Eosin (H&E) and examined under light microscope. A histological diagnosis was made including modified Bloom-Richardson histological grading and TNM (tumour (T), nodes (N), and metastases (M) staging was done wherever applicable (10),(11). The epithelial lesions were categorised into benign, premalignant or in-situ and malignant or invasive carcinomas. Phyllodes tumours were categorised into benign, borderline and malignant subtype based on histological findings. Immunohistochemical staining for CD34 was done from the preserved paraffin block using the kit, hermo scientific CD34 (Clone QBEnd/10). Each section was examined and the number of duct/lobular units was identified. The grading of CD34 expression was determined for each duct/lobular unit separately. The sections stained for CD34 were evaluated at high power (x400). Grading was done from 0 to 3+, where:

0: Upto 5% stromal cells immunoreactive
1+: >5 and upto 25% stromal cells immunoreactive
2+: >25 and upto 50% stromal cells immunoreactive
3+: >50% stromal cells immunoreactive

The staining of endothelial cells in blood vessels was taken as internal control.

Grade 0 was interpreted as complete loss of CD34
Grade 1+ was interpreted as reduced expression,

While grade 2+ and 3+ were interpreted as retained expression of CD34 (12). In the present study, Grade-0 and Grade-1 were considered as CD34 negative; and Grade-2 and Grade-3 were considered as CD34 positive.

Statistical Analysis

Statistical analysis was done using Statistical Package for the Social Sciences (SPSS) software version 13.0 and Student’s t-test was performed to assess the level of significance.

Results

Total 78 cases were included in the present study. All the participants were female and 62% of them were more than 45 years old. Of these 50 (64.1%) were benign and rest 28 (35.9%) cases were either premalignant in-situ carcinomas or invasive malignant neoplasms. Most common benign lesion was fibroadenoma (34%) and the most common malignant tumour was invasive carcinoma of no special type (39.3%) (Table/Fig 1). Out of total 28 cases of malignant breast tumours included in the present study, 15 cases (53.6%) presented with regional lymph node metastasis. Among malignant tumours, nine cases were in clinical stage 0 whereas 14 cases were classified as stage II and five cases were categorised as stage III tumour. On histological grading of 11 cases of invasive carcinoma of no special type, 1 case (9.09%) was categorised as grade 1, 6 cases (54.55%) as grade 2 and 4 cases (36.36%) as grade 3 lesions with grade 2 tumour being the most common type (Table/Fig 2). All the cases were subjected to CD34 staining. (Table/Fig 1) shows the distribution of different breast lesions in the study population and their intensity of CD34 staining in stromal cells. Most of the benign tumour showed Grade 3 positivity in stromal cells. (Table/Fig 3) is showing Grade 3+ staining in a case of fibroadenoma. However, out of two cases of fibroadenoma with focal Atypical Ductal Hyperplasia (ADH) showed reduced staining intensity for CD34 in the area of ADH as represented by Grade 1+ and Grade 2+ staining pattern. Among the three cases of ADH, 1 case was negative (Grade1+) and 2 cases were positive (Grade 2+). Cases of apocrine metaplasia also showed reduced expression of CD34. Cases of Ductal Carcinoma In-Situ (DCIS) showed higher frequency of loss of CD34 expression compared to Lobular Carcinoma In-Situ (LCIS) (83.33% vs 66.67%). Complete loss of CD34 expression was found in most of the invasive malignant neoplasms except a single case of malignant phyllodes tumour showed retention of CD34 staining (Grade 2+). (Table/Fig 4) is showing complete loss of CD34 staining in a case of malignant phyllodes tumour.

The difference in CD34 expression between benign and both in-situ and invasive malignant tumours were found to be statistically extremely significant (p<0.001) whereas those between borderline and malignant phyllodes found to be statistically non-significant (p-value 0.342). Among tumours of epithelial origin, in-situ carcinomas show statistically significant (p-value=0.0146) retention of CD34 expression in stromal cells compared to invasive carcinomas. As all the cases of invasive carcinoma of no special type showed complete loss of CD34 expression in stromal cells (Table/Fig 5) (Grade 0) 38irrespective of their histological grade, it can be concluded that CD34 expression cannot help to differentiate breast carcinomas of different histological grade. No statistically significant difference in CD34 expression was noted among tumours of different clinical stages (p-value >0.05). However, malignant tumours without metastasis in regional lymph node showed statistically significant (p<0.05) higher grade of CD34 expression compared to those with lymph node metastasis.

Discussion

Breast cancer is the most common cancer among women. Life time risk of breast carcinoma is one in every 10 women (13). Prognosis of breast cancer largely depends on early diagnosis. Better understanding of underlying molecular and cellular basis of tumour progression can help in early diagnosis and also to develop target therapy in breast carcinomas. The role of stromal microenvironment in tumour progression has long been discussed in relation to various tumours. The stroma surrounding the tumour greatly differs from normal stroma with alteration in protein synthesis and it regulates the proliferation of epithelial component of the tumour (14),(15),(16). Progression of in-situ to invasive carcinoma is an important yet poorly understood area of tumour progression. So differentiating DCIS and LCIS from benign and invasive carcinoma is critically important as earlier diagnosis is the most important step in the management of breast carcinoma. Though histology is considered as the gold standard for diagnosis of breast tumour, but immunohistochemical study has proven to play indispensible role when there is a diagnostic dilemma as often experienced by histopathologists. CD34 is a transmembrane glycoprotein expressed by many cells in our body like haematopoietic stem cells, endothelial cells and messenchymal cells of various organs including stromalfibrocytes of breast. They play a major role in cell adhesion, signal transduction and matrix substance production. It has also been claimed that CD34 molecule may also play role in host response to tissue injury [3,17]. Previous studies have shown that loss of CD34 staining in stromal cells may help to distinguish malignant from benign tumours of skin and gastrointestinal tract [18-20]. Recent studies have also proposed the feasibility of targeting tumour stroma including fibroblasts derived factors for treatment of cancer (3). The present study was conducted to assess the role of CD34 in differentiating benign lesions from borderline and malignant tumours of breast. Most of the tumours evaluated in present study were benign comprising 64.1% of all tumours with fibroadenoma being the most common type (34%). Malignant and premalihnant tumours constituted 35.9% of the cases with invasive carcinoma of no special type as the major tumour type (39.3%). Distribution of breast tumours found in this study was in concordance with the previous study done by Cimpean AM et al., (2). In the present study, most of the benign lesions of breast showed Grade 3+ staining for CD34 in stromal cells except three cases of apocrine metaplasia, three cases of ADH and in the focal area of ADH in two cases of fibroadenoma showed Grade 1+ to Grade 2+ staining with positivity rate being 66.67% each for first two categories and 50% for the last one respectively. The finding of the present study was comparable to the previous study by Khan AA et al., (12). They also observed Grade 2+ to Grade 3+ staining pattern of CD34 in 96% of the cases of ADH (12). Chauhan H et al., demonstrated diffuse loss of CD34 expression in 50% cases of ADH which is similar to this study (9). Cimpean AM et al., found retention of CD34 positivity in 100% cases of fibroadenoma with ADH with decreased intensity in their study (2). Reduced expression of CD34 in the areas of ADH may be indicative of the premalignant nature of the lesion. Similar to this study Khan AA et al., also found reduced intensity of CD34 staining in cases of apocrine metaplasia as represented by Grade 2+ to Grade 3+ staining in only 53.33% cases compared to 66.67% cases in the present study (12). The present study depicted statistically significant (p<0.001) loss of CD34 expression in stromal cells of in-situ carcinomas compared to benign lesions indicating their premalignant behaviour. In the present study, out of six cases of DCIS and three cases of LCIS, only two cases including one case from each sub-type showed retention of CD34 expression (Grade 2+). So in the present study, 33.33% cases of LCIS showed CD34 expression. This finding was comparable with Cimpean AM et al., and Chauhan H et al.,they also found retention of CD34 expression in all cases of LCIS [2,9]. Khan AA et al., found CD34 expression in 88.5% of LCIS cases (12). It has been observed that 20-30% cases of LCIS develop invasive carcinoma subsequently (21). This indicates the premalignant nature of LCIS which is corroborative with the loss of CD34 staining in a substantial population of cases in the present study. The relation between pattern of CD34 expression and DCIS was found to be variable in different studies. (Table/Fig 6) demonstrating the comparison of CD34 expression pattern in DCIS as found by present and previous studies (2),(8),(9),(12). So, it was found that CD34 expression in DCIS found in current study was comparable to the pattern observed in high grade DCIS particularly in previous studies. Irrespective of the histological sub-type, all categories of invasive carcinomas including invasive carcinoma of no special type, lobular carcinomas, tubular carcinoma, medullary carcinoma showed complete loss of CD34 staining in stromal cells. This finding was in concordance with previous studies (4),(5),(8),(17),(20). The present study and Cimpean AM et al., found less marked loss of stromal CD34 expression in invasive lobular carcinoma compared to Invasive Ductal Carcinoma (IDC) (2). In contrast Kuroda N et al., found similar frequency of CD34 loss in both IDC and ILC (22). The intensity of CD34 expression was found to be significantly higher in-situ carcinomas compared to invasive carcinomas with p-value <0.05. It was concluded that CD34 staining can be utilised to differentiate in-situ from invasive carcinomas when histology alone is inconclusive. In the present study, stromal expression of CD34 was found among 100%, 50% and 33.33% of benign, borderline and malignant phyllodes tumour respectively. Cimpean AM et al., also found loss of CD34 expression in malignant phyllodes tumour (2). There was a statistically significant difference in CD34 expression among benign and borderline phyllodes tumour, however the difference was not statistically significant between borderline and malignant phyllodes tumour. So, it was concluded that though CD34 staining can be used to differentiate benign phyllodes from borderline or malignant tumours, but it cannot be utilised to differentiate borderline from malignant phyllodes tumour. Overall, the difference in CD34 expression among benign and malignant tumours of breast was found to be highly statistically significant (p<0.001) which was similar to the observation noted by Khan AA et al., (12). Statistically significant higher intensity of CD34 staining was also noted in carcinomas without regional lymph node metastasis compared to those with lymph node metastasis (p-value <0.05). However, no significant association was found with the histological grade and clinical stage of the tumour.

To summarise, statistically significant (p<0.05) difference in extent of CD34 staining was noted among benign, in-situ and invasive malignant epithelial tumours of breast. So, it can be utilised for differentiating benign from in-situ and in-situ from invasive malignant tumours, especially when there is a diagnostic dilemma on routine histology. However, there was no statistically significant difference in intensity of CD34 expression among borderline and malignant phyllodes tumour in the present study.

Limitation(s)

Acquisition of α-SMA expression in stromal cells of malignant tumours of breast which is indicative of myofibroblastic differentiation of stromal fibrocytes could not be evaluated in the present study.

Conclusion

It was concluded that, CD34 can play crucial role in differentiating benign from in-situ and in-situ from invasive malignant epithelial tumours of breast. It can also be used to differentiate benign from malignant phyllodes tumour of breast, but its role in differentiating borderline from malignant phyllodes tumour is limited.

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Tables and Figures

[Table / Fig - 1] [Table / Fig - 2] [Table / Fig - 3] [Table / Fig - 4] [Table / Fig - 5]

DOI and Others

DOI: 10.7860/JCDR/2022/55414.16241

Date of Submission: Feb 08, 2022
Date of Peer Review: Mar 05, 2022
Date of Acceptance: Mar 17, 2022
Date of Publishing: Apr 01, 2022

AUTHOR DECLARATION:
• Financial or Other Competing Interests: None
• Was Ethics Committee Approval obtained for this study? Yes
• Was informed consent obtained from the subjects involved in the study? Yes
• For any images presented appropriate consent has been obtained from the subjects. Yes

PLAGIARISM CHECKING METHODS:
• Plagiarism X-checker: Feb 10, 2022
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• iThenticate Software: Mar 11, 2022 (9%)

ETYMOLOGY: Author Origin

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