1.CD133 marks for colorectal adenocarcinoma
Man-Fong Chew ; Kean-Hooi Teoh ; Phaik-Leng Cheah
The Malaysian Journal of Pathology 2012;34(1):25-28
CD133, a marker which has been advocated to mark colorectal carcinoma “stem or tumour initiating
cells” is amongst the frequently studied markers in colorectal cancer. A study was conducted at
the Department of Pathology, University of Malaya Medical Centre to determine the expression of CD133 in 56 archived, formalin-fi xed, paraffi n-embedded colorectal adenocarcinoma in comparison with adjacent benign colorectal epithelium by immunohistochemical staining for CD133 expression. CD133 immunopositivity was determined as staining at the glandular luminal surface or in the
intraluminal debris. Expression was semiquantitated for (1) proportion of CD133 immunopositivity in the malignant or adjacent benign colorectal epithelium and (2) intensity of staining. The fi nal score of CD133 immunopositivity was arbitrarily taken as proportion of CD133 immunopositivity multiplied by intensity of staining in both the malignant and adjacent benign colorectal epithelium.CD133 expression was observed in signifi cantly increased frequency in 49 (87.5%) colorectal
adenocarcinoma compared with 15 (26.8%) of the adjacent benign colorectal epithelium (p<0.05). In terms of immunopositivity score (proportion of CD133 immunopositivity multiplied by intensity of staining), colorectal adenocarcinoma had a mean arbitrary score of 8.5 which was signifi cantly higher than the mean immunopositivity score of 0.5 of the adjacent benign colorectal epithelium (p<0.05). In addition, the maximum immunopositivity score for the adjacent benign colorectal
epithelium was 4, while 38 (67.9%) of colorectal adenocarcinoma had scores >4. This study shows
that CD133 is able to mark colorectal adenocarcinoma but it is still unclear at this juncture whether
CD133 is indeed a marker for colorectal adenocarcinoma “stem cells”.
2.E-cadherin downregulation at the infiltrating tumour front is associated with histological grade and stage in colorectal carcinoma of Malaysians
Serena Diane Dass ; Phaik-Leng Cheah ; Diana Bee-Lan Ong ; Kean-Hooi Teoh ; Lai-Meng Looi
The Malaysian Journal of Pathology 2015;37(1):19-24
Loss of E-cadherin, a 120 kDA transmembrane glycoprotein responsible for cell-cell adhesion,
is one of the hallmarks of epithelial-mesenchymal-transition (EMT). E-cadherin expression was
immunohistochemically studied in 94 histopathologically re-confirmed colorectal carcinomas (CRC)
using a monoclonal antibody to E-cadherin (Dako: Clone NCH-38) on a Ventana Benchmark XT
automated system. Each case was assessed for E-cadherin immunopositivity at two separate locations
viz the tumour centre (TC) as well as the infiltrating front (IF). Expression was semiquantitated
for proportion of immunopositive malignant cells as 0 (negative), 1 (1-25% staining), 2 (26-50%
staining), 3 (51-75% staining) and 4 (>75% staining) and staining intensity: 0 (negative), 1 (weak),
2 (moderate) and 3 (strong). The final histoscore of E-cadherin immunopositivity was arbitrarily
computed as proportion of immunopositivity multiplied by staining intensity of the malignant cells.
E-cadherin histoscores were significantly lower at the IF (4.5 ± 2.5) compared with TC (10.7 ± 2.4).
Furthermore, the histoscores were significantly reduced at the IF of 49 TNM III+IV tumours (3.6 ±
2.5) compared with 45 II+III CRC (5.4 ± 2.2). Reduction of E-cadherin expression was also noted
in the 23 high grade (TC=8.6 ± 3.2; IF=2.6 ± 2.3) compared with 71 low grade tumours (TC =
11.4 ± 1.5; IF = 5.1 ± 2.3). E-cadherin is downregulated at the infiltrating front of CRC, possibly
marking for EMT at this location. The downregulation is further enhanced amongst late stage and
high grade tumours compared with earlier stage and low grade tumours; findings which are similar
to that noted in CRC of other populations.
3.Implications of continued upregulation of p16INK4a evolution from high-grade squamous intraepithelial lesion to invasive squamous carcinoma of the cervix
Phaik-Leng CHEAH ; Lai-Meng LOOI ; Kein-Seong MUN ; NAZARINA ; Kean-Hooi TEOH
The Malaysian Journal of Pathology 2011;33(2):83-87
On integration into the host cervical keratinocyte genome, human papillomavirus (HPV) E7 protein
binds pRB, releasing E2F from normally incompetent pRB-E2F complexes and allowing propagation
of G1-S transition by the E2F. p16 INK4a, a tumour suppressor protein, increases in refl ex response to
counter this. 29 histologically re-confi rmed low-grade squamous intraepithelial lesions (LSIL), 27
high-grade squamous intraepithelial lesions (HSIL) and 30 invasive cervical squamous carcinoma
(SCC) were immunohistochemically stained for p16INK4a expression using the CINtec Histology Kit
(REF 9511, mtm laboratories AG, Heidelberg, Germany) to re-affi rm the notion that integration
of HPV occurs predominantly in SCC and possibly HSIL and less in LSIL and normal squamous
epithelium (NSqE). Implicit was also the attempt to understand the role of E2F, as indicated by
p16INK4a, in evolution of SCC from HSIL. No ethnic predilection was noted for LSIL, HSIL or SCC.
Patients with SCC were signifi cantly older by about 14-years compared with HSIL (p<0.05) while
there was no signifi cant age difference between HSIL and LSIL. p16INK4a expression was signifi cantly
increased (p<0.05) in both HSIL (88.9%) and SCC (83.3%) compared with LSIL (3.4%) and NSqE
(0%); the NSqE being normal squamous epithelium noted in 17 of the LSIL, 19 HSIL and 5 SCC.
From these fi ndings there is suggestion that fundamental upstream events viz HPV integration, E7
upregulation followed by E2F activation occurs at point of transformation to HSIL and continues
unrelentingly for another one to two decades before hitherto unclear factors convert a non-invasive
lesion into an overtly invasive malignant counterpart. Interestingly, the occurrence of HSIL and
LSIL in almost the same age group could mean that alteration from episomal to integrated form of
HPV may not incur a prolonged incubation period, unlike from HSIL to SCC
4.An analysis of predictive biomarkers in routine histopathological reporting of infi ltrating ductal breast carcinoma in a tertiary hospital in Malaysia with a focus on limitations and directions for future development
Kean-Hooi TEOH ; Lai-Meng LOOI ; Subathra SABARATNAM ; Phaik-Leng CHEAH ; Abdul Rahman NAZARINA ; Kein-Seong MUN
The Malaysian Journal of Pathology 2011;33(1):35-42
Predictive biomarkers such as oestrogen (ER) and progesterone (PR) receptors and c-erbB-2
oncoprotein have become a staple in breast cancer reports in the country as they increasingly
play an important role in the treatment and prognosis of women with breast cancers. This study
reviews the practice of histopathology reporting of these biomarkers in a Malaysian tertiary hospital
setting. Retrospective data on demographic, pathological and biomarker profi les of patients with
invasive ductal carcinoma who had undergone mastectomy or lumpectomy with axillary node
clearance from 2005 to 2006 were retrieved from the Department of Pathology, Penang Hospital
and analysed. The prevalence of ER positivity (55.8%), PR positivity (52.5%), c-erbB-2 oncoprotein
overexpression (24%) and triple negativity (ER negative, PR negative, c-erbB-2 negative) (15%)
by immunohistochemistry were comparable with other studies. Notably, c-erbB-2 overexpression
was equivocal (2+) in 15% of cases. Since about a quarter of equivocal (2+) cases usually show
amplifi cation by FISH, a small but certain percentage of patients would miss the benefi t of anti-cerbB-
2 antibody therapy if FISH is not performed. New ASCO/CAP guidelines on the quantitation
of ER and PR will probably increase the prevalence of ER/PR positivity, invariably leading to
signifi cant ramifi cations on the management of patients as more patients would be deemed eligible
for endocrine therapy, as well as categorisation of triple negative breast cancers.
5.Leptomeningeal glioblastoma multiforme presenting as cauda equina syndrome
Mei-Ling Sharon Tai ; Kartini Rahmat ; Kean Hooi Teoh ; Ravindran Karuppiah ; Hazman Mohd Nor ; Fatimah Kamila Abu Bakar ; Chong Tin Tan
Neurology Asia 2014;19(2):227-230
Glioblastoma multiforme (GBM) is the commonest primary cerebral malignancy consisting of 12- 20% of intracranial brain tumours.1 We report here a patient with GBM with very unusual marked and widespread leptomeningeal GBM.