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"ABSTRAKLatar Belakang : Paduan kemoterapi berbasis platinum dengan generasi ketiga khususnya karboplatin-vinorelbin sudah sering digunakan sebagai kemoterapi paliatif pada pasien KPKBSK stage lanjut di Indonesia khususnya Rumah Sakit Umum Pusat RSUP Persahabatan namun sampai saat ini belum terdapat data mengenai efikasi dan toksisiti paduan kemoterapi ini di RSUP Persahabatan.Metode : Desain penelitian ini adalah survey observasional retrospektif pada pasien KPKBSK stage lanjut IIIB dan IV yang menjalani kemoterapi lini I di RSUP Persahabatan dengan paduan kemoterapi karboplatin-vinorelbin sejak 1 Januari 2015 sampai 30 Maret 2017.Hasil : Total subjek dalam penelitian ini adalah 38 pasien yang mendapatkan paduan kemoterapi Karboplatin AUC-5 pada hari ke-1 dan vinorelbin 30 mg/m2 pada hari ke1 dan ke-8. Paduan kemoterapi karboplatin-vinorelbin mempunyai efikasi yang baik dengan Objective overall response rate ORR 12,5 dan clinical benefit rate CBR 87,5 . Overall survival OS pada penelitian ini adalah 34,2 dengan masa tengah tahan hidup 387 hari 12,9 bulan dan progression free survival 323 hari 10,7 bulan. Toksisiti hematologi dan nonhematologi yang paling sering terjadi adalah anemia derajat 1 38,4 dan keluhan mual, muntah derajat 2 57,9 . Pada penelitian ini terdapat 2 kasus perdarahan saluran cerna derajat 2 namun pasien masih dapat melanjutkan kemoterapi. Kami juga mendapatkan komplikasi tindakan kemoterapi berupa phlebitis ringan pada 24 pasien 65,7 dan phlebitis sedang pada 1pasien 2,6 .Kesimpulan: Paduan karboplatin-vinorelbin sebagai kemoterapi lini I memiliki efikasi yang baik serta efek toksisiti yang masih dapat ditoleransi sehingga aman diberikan pada pasien KPKBSK stage lanjut. Kata kunci: efikasi, toksisiti, hematologi, nonhematologi, objective overall response rate, clinical benefit rate, overall survival, MTTH, TTP, PFS

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ABSTRAK Background Combination of platinum base and third generation drugs Carboplatin and vinorelbine chemotherapy are frequently used as paliative chemotherapy for Non small cell lung cancer NSCLC patients in Indonesia especially in Persahabatan Hospital. But there are still no data about the activity and tolerability of this regiment in Persahabatan Hospital. This study is conducted to evaluate the efficacy and toxicity of this regiment as first line chemotherapy for advanced NSCLC patients in Persahabatan Hospital.Method This study is an observational survey retrospective study for advanced NSCLC patientswho receive carboplatin vinorelbine regiment as fisrt line chemotherapy since 1st January 2015 to 30th March 2017.Result We observea total of 38 patients who receive carboplatin 5 AUC on day 1 and vinorelbine 30mg m2 on day 1 and 8. This regiment has a good efficacy with overall response rate ORR 12,5 and clinical benefit rate CBR 87,5 . The overall survival OS is 34,2 with median of survival time 387 days 12,9 moths and PFS 323 days 10,7 moths . We found grade 1 anemia 38,4 and grade 2 nausea vomiting 57,9 as hematological and non hematological toxicity that frequently occur in this study. We found 2 cases of grade 2 gastrointestinal bleeding but the patients are still able to continue the chemotherapy after doing some correction for the haemoglobin Hb . We also found mild phlebitis in 24 patients 65,7 and 1 moderate phlebitis in 1 patient 2,6 as procedural complication of this chemotherapyConclusion Combination ofcarboplatin and vinorelbine as first line chemotherapy has a good efficacy and tolerability for advanced NSCLC patients. Key word efficacy, toxicity, haematological, non hematological, overall objective response rate ORR , clinical benefit rate CBR , overall survival OS , median time of survival, time to progression TTP and progression free survival PFS ."

"Latar belakang: Meningkatnya insidens kesakitan dan kematian akibat keganasan alternatif terapi dengan kemoterapi. Rejimen kemoterapi menggunakan obat sitotoksik yang mempunyai batas terapi sangat sempit sehingga memberi efek samping lebih besar dibandingkan manfaat dan angka harapan hidup. Kedua hal ini terjadi pada pasien KPKBSK jenis KSS dan adenokarsinoma EGFR wild type. Metode: Desain penelitian ini dilakukan dengan metode Survey retrospektif dan studi analitik terhadap faktor yang mempengaruhi prognosis. Data diambil dari Rekam Medis RSUP Persahabatan dengan total sampling pada periode 2011 sampai 2016. Hasil: Sampel penelitian teridiri dari 30 subjek kelompok KSS dan 30 subjek kelompok adenokarsinoma dengan karakteristik subjek laki-laki 86,7% dan subjek perempuan 13,3% dengan usia (median 57, range 36-66). Mendapatkan median TTP pada kelompok KSS yaitu 150 Hari (IK 95% 123,401-176,599) dan adenokarsinoma memiliki TTP 150 Hari (IK 95% 134,818-165,182).Mendapatkan KSS memiliki median PFS 150 Hari (IK 95% 99,790-200,210) dan adenokarsinoma memiliki PFS 150 Hari (IK 95% 121,597-178,403). Mendapatkan median KSS memiliki median OS 330 Hari (IK 95% 265,558-349,412) dan adenokarsinoma memiliki OS 341 Hari (IK 95% 227,930-404,070). Subjek dengan one year survival rate pada kedua kelompok sama banyak yaitu 47%. Kejadian anemia terbanyak yaitu grade 2 pada kelompok KSS sebanyak 8 subjek dan kelompok adenokarsinoma EGFR wild type sebanyak 5 subjek. Kesimpulan:Perbandingan Efikasi dan toksisitas hematologi kemoterapi lini I kanker paru karsinoma bukan sel kecil (KPKBSK) jenis karsinoma sel skumosa (KSS) dengan adenokarsinoma EGFR wild typetidak mengalami perbedaan yang signifikan.

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Background:The increasing incidence of morbidity and mortality is due to malignancy alternative therapy using chemotherapy. Chemotherapy using cytotoxic agents with narrow margin of safety results in greater side effects and decreasing chance of survival that occur in squamous cell carcinoma and wild-type EGFR adenocarcinoma.

Methods: This is a retrospective survey and analytic study of factors that affect prognosis. Data was obtained from patients’ medical records in RSUP Persahabatan from 2011 to 2016.

Results: The subjects of this study consist of 30 patients with squamous cell carcinoma (SCC) and 30 patients with wild-type EGFR adenocarcinoma, 86,7% of the subjects are male and 13,3% are female with median age 57 (range 36-66). Median TTP in SCC is 150 days (CI 95% 123,401-176,599) and in adenocarcinoma is 150 days (CI 95% 134,818-165,182). Progression free survival in SCC is 150 days (CI 95% 99,790-200,210) and in adenocarcinoma is 150 days (CI 95% 121,597-178,403). Median OS of SCC is 330 days (CI 95% 265,558-349,412) and adenocarcinoma is 341 days (CI 95% 227,930-404,070). One year survival rate subjects in those two groups are similar, which is 47%. Highest incidence of anemia is grade 2 anemia in 8 subjects with SCC and 5 subjects with adenocarcinoma.

Conclusion: First-line chemotherapy has similar efficacy and toxicity both in patient with NSCLC-SCC and NSCLC-wild type EGFR adenocarcinoma."

"Latar Belakang: Tingginya angka kejadian kanker paru menyebabkan diperlukan pemanfaatan suatu penanda biologis spesifik kanker paru untuk menilai progresifitas penyakit. Transforming growth factor-β adalah protein yang disekresi untuk meregulasi proliferasi, diferensiasi dan kematian dari berbagai jenis sel. Semua jenis sel kekebalan termasuk sel B, sel T, sel dendritik dan makrofag mensekresi TGF-β. Jenis TGF-β yang terbanyak adalah TGF-β1. Diperlukan pengukuran kadar TGF-β1 serum darah tepi sebagai faktor prognostik pada kanker paru khususnya KPKBSK stage lanjutMetode: Penelitian ini merupakan studi perbandingan dengan disain potong lintang pada pasien kanker paru yang telah tegak diagnosis dan bersedia diambil serum darah tepi untuk pemeriksaan kadar TGF-β1 serum menggunakan Human TGF-β1 Quantikine ELISA kit dari R D. Kadar TGF-β1 serum diukur pada 68 subjek yang terdiri dari 30 subjek kelompok kanker paru dan 38 subjek kelompok bukan kanker paru.Hasil: Kadar TGF-β1 serum pada kelompok kanker paru meningkat signifikan lebih tinggi dibandingkan kelompok bukan kanker paru (median; min-max) (3601.85; 2006.87-14995.25 pg/mL vs 2510.11; 646.31-5584.07 pg/mL) (P = 0.000). Tidak ditemukan hubungan antara kadar TGF-β1 serum dengan jenis kelamin, umur, riwayat merokok, gejala klinis, gambaran bronkoskopi, jenis sitologi/histopatologi, KPKBSK stage lanjut, dan status tampilan umum. Median Survival Time (95% CI) TGF-β1 < 3601.85 pg/mL adalah 9.7 (2.4-16.9) bulan sedangkan TGF-β1 ≥ 3601.85 pg/mL adalah 16.7 (7.7-25.7) bulan. Over all survival TGF-β1 13.3 (5.8-20.8) bulanKesimpulan: Kadar TGF-β1 serum meningkat pada kelompok kanker paru dibandingkan kelompok bukan kanker paru. Kadar TGF-β1 serum belum dapat digunakan sebagai marker prognostik kanker paru.

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Beckground: The high incidence rate of lung cancer leads to the utilization of a specific biological marker of lung cancer to assess disease progression. Transforming growth factor-β is a secreted protein to regulate the proliferation, differentiation and death of different cell types. Types of immune cells are B cells, T cells, dendritic cells and macrophages secreting TGF-β. The most common type of TGF-β is TGF-β1. Therefore, measurement of serum level of TGF-β1 as a prognostic factors in lung cancer, especially advanced stage NSCLC, to assess progressivity of lung cancer is needed. Method: This study is a comparative study with cross-sectional design in lung cancer patients who had been diagnosed and were willing to be taken for examination of peripheral blood serum levels of TGF-β1 using the Quantikine Human TGF-β1 ELISA kit from R&D system. TGF-β1 serum levels were measured in 68 subjects consisted of 30 subjects with lung cancer group and 38 subjects controlled group. Result: Serum level of TGF-β1 in lung cancer group increased significantly higher than control group (median; min-max) (3601.85; 2006.87-14995.25 pg/mL vs. 2510.11; 646.31-5584.07 pg/mL) (P = 0.000). There was no association between serum level of TGF-β1 with gender, age, smoking history, clinical symptoms, bronchoscopy, cytology/histopathology, advanced stage of NSCLC, and performance status. Median Survival Time (95% CI) TGF-β1 <3601.85 pg/mL was 9.7 (2.4-16.9) months while TGF-β1 ≥ 3601.85 pg/mL was 16.7 (7.7-25.7) months. Over all survival TGF-β1 13.3 (5.8-20.8) months. Conclusion: Serum level of TGF-β1 is higher in the lung cancer group compared to controlled group. Serum TGF-β1 levels can not be used as a prognostic markers of lung cancer."

"ABSTRAK Tesis ini menilai efikasi dan toksisiti Erlotinib/Gefitinib sebagai terapi lini kedua pada pasien KPKBSK yang mengalami progresifitas. Ini adalah sebuah penelitiankohor retrospektif antara tahun 2009 sampai 2013 dari rekam medis pasienKPKBSK yang mengalami progresifitas. Respons (subjektif, semisubjektif danobjektif) dievaluasi setiap bulan. Toksisiti dinilai setiap minggu sejak pemberianErlotinib/Gefitinib berdasarkan kriteria WHO. Hasil evaluasi respons objektif,tidak ada pasien yang memberikan respons komplit. Best overall response ratedari 31 pasien, 48,8% menetap, 22,6% perburukan,12,9% respons sebagian dan6,5% tidak dinilai/inevaluable. Pada penilaian respons semisubjektif didapatkan19.4% peningkatan berat badan, 51,6% penurunan berat badan dan 29,0%menetap. Waktu tengah tahan hidup mencapai 18 bulan, rerata masa tahan hidup1 tahunan 80,6% dan masa tahan hidup keseluruhan 6,50%. Data menunjukkantidak ada timbul toksisiti hematologi berat (grade ¾) dan data penilaian toksisitinon hematologi sangat jarang timbul toksisiti berat (grade ¾). Efikasi monoterapiEGFR-TKI (Erlotinib/Gefitinib) cukup tinggi dengan toksisiti yang ditimbulkantidak berat. Dengan demikian Erlotinib/Gefitinib sebagai terapi lini kedua cukupbaik.ABSTRACT This thesis assesses the efficacy and toxicity of Erlotinib/Gefitinib as a second

line therapy in NSCLC patients. This is a retrospective cohort study between 2009

and 2013 from the medical records of patients who experienced progression

NSCLC. Therapeutic response was evaluated every month. Toxicity assessed

every month since giving Erlotinib/Gefitinib according to WHO?s criteria. Results

of objective response evaluation none of the patients complete response. Best

overall response rate of 31 patients with the most stable response are 48.8%. Most

semisubjective response obtained are 51.6% weight loss. The middle survival time

reached 18 month, the mean 1 year survival time are 80.6% and a 6.50% overall

survival. The data showed no hematologic toxicity arise severe (grade ¾) and

non-hematological toxicity very rarely arise severe toxicity. The efficacy of EGFR

TKI monotherapy (Erlotinib/Gefitinib) is high enough with toxicity cause not

severe. Thus Erlotinib/Gefitinib as second-line therapy is quite good. ;This thesis assesses the efficacy and toxicity of Erlotinib/Gefitinib as a second

line therapy in NSCLC patients. This is a retrospective cohort study between 2009

and 2013 from the medical records of patients who experienced progression

NSCLC. Therapeutic response was evaluated every month. Toxicity assessed

every month since giving Erlotinib/Gefitinib according to WHO?s criteria. Results

of objective response evaluation none of the patients complete response. Best

overall response rate of 31 patients with the most stable response are 48.8%. Most

semisubjective response obtained are 51.6% weight loss. The middle survival time

reached 18 month, the mean 1 year survival time are 80.6% and a 6.50% overall

survival. The data showed no hematologic toxicity arise severe (grade ¾) and

non-hematological toxicity very rarely arise severe toxicity. The efficacy of EGFR

TKI monotherapy (Erlotinib/Gefitinib) is high enough with toxicity cause not

severe. Thus Erlotinib/Gefitinib as second-line therapy is quite good. "