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Hartono Tjahjadi
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Penggunaan Pulasan Imunohistokimia p53, Ki67 dan Epidermal Growth Factor Receptor (EGFR) dalam Membedakan Adeno-karsinoma Serosum Ovarium Tipe I (Low grade) dan Tipe II (High grade) Hartono Tjahjadi; Tantri Hellyanti
Majalah Patologi Indonesia Vol 24 No 1 (2015): MPI
Publisher : Perhimpunan Dokter Spesialis Patologi Indonesia (IAPI)

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ABSTRAK Latar belakang Adenokarsinoma serosum ovarium tipe II (high grade) lebih sering ditemukan dibandingkan tipe I (low grade). Tumor tipe II bersifat agresif, namun lebih sensitif kemoterapi. Hal sebaliknya terjadi pada tumor tipe I. Mutasi p53 berperan dalam patogenesis berbagai jenis keganasan, termasuk organ genitalia wanita. Ki67 terlibat dalam semua fase aktif pada siklus sel (G1, S, G2 dan mitosis). EGFR mengaktifkan jalur sinyal yang menginduksi onkogenesis dan proliferasi sel. Tujuan penelitian ini untuk mengetahui peran p53, Ki67 dan EGFR dalam patogenesis adenokarsinoma serosum ovarium dan peluang penggunaannya sebagai alat bantu diagnostik untuk membedakan tumor tipe I dan tipe II. Metode Penelitian observasional analitik potong lintang, pada 25 kasus adenokarsinoma serosum ovarium dari arsip Departemen Patologi Anatomik FKUI/RSCM 2011-2013, dengan bahan blok parafin. Dilakukan pulasan imunohistokimia p53, Ki67 dan EGFR dengan metode indirect. Pada kedua kelompok dihitung dan dibandingkan persentase positivitas pulasan inti p53 dan Ki-67, serta H score ekspresi EGFR. Hasil Median ekspresi p53, Ki67 dan H score EGFR pada kelompok tipe I adalah 15 (4-50), 15 (5-30), dan 46,5 (30-180); sedangkan pada tipe II adalah 80 (0-90), 20 (10-60), dan 40 (0-160). Perbandingan ekspresi p53, Ki67 dan H score EGFR pada kedua kelompok tumor: p=0,03, 0,37 dan 0,05. Kesimpulan Protein p53 berperan penting dalam patogenesis adenokarsinoma serosum ovarium tipe II (high grade). Ekspresi p53 dapat digunakan untuk membedakan adenokarsinoma serosum tipe II dari tipe I, sedangkan ekspresi Ki67 maupun EGFR tidak. Kata kunci: adenokarsinoma serosum, EGFR, Ki-67, ovarium, p53. ABSTRACK Background Serosum ovarian adenocarcinoma tipe II (high grade) is more common than type I (low grade). Type II tumors are aggressive, but more sensitive to chemotherapy. The opposite occurs in tumor type I. p53 mutation plays a role in the pathogenesis of a variety of malignancies, including female genital organs. Ki67 actively involved in all phases of the cell cycle (G1, S, G2 and mitosis). EGFR activate signaling pathways that induce oncogenesis and cells proliferation. The aim of this study are to determine the role of p53, Ki67 and EGFR in the pathogenesis of serosum ovarian adenocarcinoma and to determine the possibilities to use them as diagnostic tool to differentiate tumor type I and type II. Methods A consecutive cross-sectional observational study, in 25 cases of serosum ovarian adenocarcinoma from archives in Department of Anatomical Pathology Faculty of Medicine University of Indonesia/RSCM 2011-2013, with material paraffin blocks. Indirect immunohistochemical staining of p53, Ki67 and EGFR were performed. Results in both groups were calculated and compared the percentage of core outward positivity p53 and Ki-67, and H scores EGFR expression. Results Median expression of p53 , Ki67 and EGFR score in group H type I was 15 (4-50), 15 (5-30), and 46.5 (30-180); where as in type II was 80 (0-90), 20 (10-60), and 40 (0-160). Comparison of expression of p53, Ki67 and H score of EGFR in both tumor groups: p=0.03, 0.37 and 0.05 . Conclusions P53 protein plays an important role in the pathogenesis of type II serosum ovarian adenocarcinoma (high grade). P53 expression can be used to distinguish the type II adenocarcinoma serosum of type I, neither the EGFR nor Ki-67 expressions can be used. Key words : EGFR, Ki67, ovarian, p53, serosum adenocarcinoma.
Deteksi Mikrometastasis pada Bulky Kelenjar Getah Bening Karsinoma Serviks Stadium IA-IIB Menggunakan Sitokeratin AE1/AE3 Reni Angeline; Hartono Tjahjadi; Puspita Eka Wuyung
Majalah Patologi Indonesia Vol 29 No 3 (2020): MPI
Publisher : Perhimpunan Dokter Spesialis Patologi Indonesia (IAPI)

Show Abstract | Download Original | Original Source | Check in Google Scholar | Full PDF (472.503 KB) | DOI: 10.55816/mpi.v29i3.441

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BackgroundCervical uterine carcinoma is a primary malignant disease of the uterine cervix. The presence or absence of metastasis in lymphnodes does not alter the stage but affects recurrence, survival, and therapy. Immunohistochemistry stains of the AE1/AE3cytokeratin can assist in the diagnosis and determine the small focus of carcinoma metastasis. In this study, we analyzedimmunohistochemistry cytokeratin AE1/AE3 could determine micrometastasis in bulky lymph nodes negative.MethodsThis study used cross-sectional design. The sample consisted of 52 cases of stage IA-IIB cervical carcinoma performed by radicalhysterectomy and lymphadenectomy accompanied by negative bulky lymph nodes at the Department of Anatomical PathologyFaculty of Medicine University of Indonesia/Cipto Mangunkusumo Hospital (FKUI/RSCM) from January 2011 to June 2017. Allcases stained by immunohistochemistry cytokeratin AE1/AE3.ResultsBulky Lymph Nodes Cervical Carcinoma stage IA-IIB, histopathologic diagnose of non keratinized squamous cell carcinoma,moderate differentiation degree, no lymphovascular invasion and deepest invasion >5.0 mm. Immunohistochemistry staining ofAE1/AE3 cytokeratin showed no micrometastasis in all cases.ConclusionThe immunohistochemistry staining of AE1/AE3 cytokeratin used in Bulky Lymph Nodes Cervical Carcinoma stage IA-IIB could notdetected micrometastasis in all cases.
Profil Klinikopatologik Karsinoma Payudara Invasif Metastasis Jauh di Departemen Patologi Anatomik FKUI/RSCM Tahun 2019 Laurencia Leny Kurnianingrum; Hartono Tjahjadi
Majalah Patologi Indonesia Vol 31 No 1 (2022): MPI
Publisher : Perhimpunan Dokter Spesialis Patologi Indonesia (IAPI)

Show Abstract | Download Original | Original Source | Check in Google Scholar | Full PDF (570.063 KB) | DOI: 10.55816/mpi.v31i1.489

Abstract

BackgroundInvasive breast carcinoma (IBC) is the highest incidence and is the leading cause of malignancy-related death in women in theworld. Bones are the most common sites of IBC metastases. This study aims to provide clinical and histological characteristic datain cases of distant metastastic IBC in the Anatomical Pathology Department, Faculty of Medicine, Universitas Indonesia, Dr. CiptoMangunkusumo General Hospital (PA-FKUI/RSCM).MethodsThis is descriptive research with cross-sectional design, using secondary data from the archives of PA-FKUI/RSCM, starting fromJanuary 1, 2019 to December 31, 2019.ResultsDistant metastases of IBC was found 65.2% as bone metastases, 46.1% as pulmonary metastases, 26.1% as liver metastases, and8.7% as brain metastases. The largest age group was 40-59 years, median age was 49 years with range 27-78 years. The mostcommon of the classification of primary tumor size was 54.8% T4, and 87% unilateral cases. Most histologic subtypes were 90.4%cases no special type, then lobular and mucinous subtypes. Lymphovascular invasion was 24.3% cases. The most commonmolecular subtype was luminal B Luminal and mostly as bone metastases and triple negative breast cancer (TNBC) in lungmetastases. The greatest histological grade was grade 2.ConclusionBone was the most common IBC metastatic. The most common of the classification of primary tumor size was T4 and histologicsubtype was no special. Luminal B was the most common molecular subtypes and the highest was bone metastases.
Co-Authors Laurencia Leny Kurnianingrum Puspita Eka Wuyung Reni Angeline Tantri Hellyanti