"Hematotoksisitas pada leukemia limfoblastik akut (LLA) anak selama terapi fase pemeliharaan, merupakan hal penting, karena dapat menyebabkan kondisi mengancam jiwa dan penghentian dini terapi, yang dapat meningkatkan risiko relaps. Untuk menghindari hematotoksisitas, American Society for Clinical Pharmacology and Therapeutics merekomendasikan penyesuaian dosis awal merkaptopurin (6MP) berdasarkan genotip enzim pemetabolisme 6MP yaitu thiopurine S-methyl transferase (TPMT), berdasarkan studi-studi sebelumnya polimorfisme enzim tersebut memengaruhi kadar metabolit aktif 6MP dan hematotoksisitas. Penelitian ini bertujuan untuk mengetahui prevalensi hematotoksisitas dan melihat hubungannya dengan genotip TPMT, fenotip TPMT, dan karakteristik pada pasien LLA anak di Indonesia. Studi potong lintang dilakukan di RS Cipto Mangunkusumo dan RS Kanker Dharmais pada bulan Juni 2017–Oktober 2018 terhadap 106 pasien LLA anak yang sedang mendapatkan 6MP minimal 1 bulan pada terapi fase pemeliharaan. Prevalensi hematotoksisitas pada fase pemeliharaan pasien LLA anak di Indonesia 71,7%, dengan neutropenia 51,9%, anemia 44,3%, dan trombositopenia 6,6%. Neutropenia tingkat 3–4 sebesar 9,4%. Alel mutan yang ditemukan hanya TPMT*3C dengan frekuensi 0,95%. Kadar 6TGN, 6MeMP dan rasio kadar 6MeMP/6TGN sangat bervariasi, yaitu 6–234,04 pmol/8x10⁸ eritrosit, 3,5–3167,01 pmol/8x10⁸ eritrosit, dan 0,06–100,64 pmol/8x10⁸ eritrosit, secara berurutan. Sebesar 76,4% pasien berusia antara 1–10 tahun dan > 95% pasien memiliki status gizi dan kadar albumin normal. Proporsi pasien berdasarkan stratifikasi risiko dan dosis harian 6MP sebanding. Tidak terdapat hubungan antara hematotoksisitas dengan genotip TPMT, usia, status gizi, kadar albumin, stratifikasi risiko, cara pemberian dosis harian 6MP, dan pemberian bersama kotrimoksazol. Faktor yang berhubungan dengan hematotoksisitas adalah fenotip TPMT: kadar 6MeMP (p = 0,004) dan rasio kadar 6MeMP/6TGN (p = 0,010). IMT ≤ 16,6 kg/m2 berhubungan dengan anemia dan kadar albumin serum ≤ 4,2 g/dL berhubungan dengan trombositopenia. Tidak terdapat hubungan antara genotip dengan fenotip TPMT pada pasien LLA anak di Indonesia. Kesimpulan: Hematotoksisitas tidak berhubungan dengan genotip TPMT dan karakteristik pasien. Fenotip TPMT berhubungan dengan hematotoksisitas, namun kurang kuat untuk memprediksi hematotoksisitas.

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Hematotoxicity in acute lymphoblastic leukemia (ALL) children during maintenance phase therapy is important, because it can cause life-threatening conditions and it is the major cause of drug discontinuation, which can increase the risk of relapse. To reduce hematotoxicity, American Society for Clinical Pharmacology and Therapeutics recommended to adjust starting dose of mercaptopurine (6MP) based on patient's genotype of thiopurine S-methyl transferase (TPMT), that affected 6MP active metabolite levels and hematotoxicity.

The aim of the study was to determine the prevalence of hematotoxicity and factors that affecting hematotoxicity, focus on genotype and phenotype of TPMT. A cross-sectional study was conducted at Cipto Mangunkusumo Hospital and Dharmais Cancer Hospital in June 2017–October 2018 for 106 LLA patients who were receiving at least 1 month of 6MP during maintenance therapy.

The prevalence of neutropenia, anemia, and thrombocytopenia were 51.9%, 44.3%, and 6.6%, respectively. We found only TPMT *3C with a frequency of 0.95%. Erythrocyte levels of 6TGN, 6MeMP, and ratio of 6MeMP/6TGN levels vary greatly, 6–234,04 pmol/8x10⁸ RBC, 3,5–3167,01 pmol/8x10⁸ RBC, and 0,06–100,64 pmol/8x10⁸ RBC. About 76.4% of patients aged 1–10 years, and > 95% of patients had normal nutritional status and serum albumin levels. The proportion of patients based on risk stratification and daily dose of 6MP were comparable. There was no association between hematotoxicity and genotype TPMT, age, nutritional status, serum albumin levels, risk stratification, daily dose of 6MP, and co-administration of cotrimoxazole. The factor associated with hematotoxicity was the TPMT phenotype: 6MeMP levels (p = 0.004) and the ratio of 6MeMP/6TGN levels (p = 0.010). BMI ≤ 16.6 kg/m2 was associated with anemia and serum albumin level ≤ 4.2 g/dL was associated with thrombocytopenia. There was no relationship between genotype and the TPMT phenotype in pediatric LLA patients in Indonesia.

Conclusion: Hematotoxicity is not associated with TPMT genotype and patient characteristics. The TPMT phenotype is associated with hematotoxicity but is not strong enough at predicting hematotoxicity."

"Pasien leukemia mieloblastik akut (LMA) yang mencapai remisi komplet pascaterapi induksi di Indonesia hanya 49%, dan event-free survival (EFS) hanya 10%. Angka kekambuhan dan kematian terkait kemoterapi menjadi penyebab rendahnya luaran tersebut. Untuk meningkatkan luaran dan mengurangi efek samping pengobatan perlu dilakukan stratifikasi risiko menggunakan profil sitogenetik maupun imunofenotipe. Tujuan penelitian ini adalah mendapatkan profil imunofenotipe, kariotipe, mutasi FLT3-ITD dan NPM1 (variabel prognosis), serta hubungannya dengan respons kemoterapi induksi.Penelitian dilakukan dengan desain kohort analitik pada LMA usia 1–18 tahun di RSCM, RSABHK, RSKAD, RSPAD pada bulan November 2018 hingga Maret 2020. Pemeriksaan yang dilakukan meliputi ekspresi CD7, CD19, kariotipe t(8,21), inv(16), mutasi NPM1 dan FLT3-ITD, kemudian dinilai hubungannya dengan kejadian remisi setelah mendapat terapi induksi dengan protokol LMA Nasional.Dari 42 subjek diperoleh median usia 8 tahun 11 bulan (3–213 bulan). Tipe LMA terbanyak adalah M1, diikuti M2. Gejala klinis tersering pucat (33/42) dan demam (25/42). Tanda klinis terbanyak hepatomegali (17/42) dan splenomegali (18/42). Subjek dengan CD7+ 21,4%, CD19+ 11,9%. Translokasi t(8;21) terdeteksi pada 1dari 18 (5,6%) subjek, inv(16) pada 4 dari 18 ((22%) subjek, 7 dari 18 subjek termasuk kelompok kariotipe favorable. Sebanyak 2 dari 28 (7%) subjek memiliki mutasi FLT3-ITD. Mutasi NPM1 tidak ditemukan. Ekspresi CD7 lebih dominan berperan dibandingkan usia dan jumlah leukosit saat diagnosis sebagai faktor prognosis baik. Analisis multivariat menunjukkan hubungan bermakna antara variabel prognosis dengan respons terapi induksi. Aberans CD7, inv(16) dan mutasi FLT3-ITD memiliki risiko relatif lebih tinggi untuk remisi (masing-masing incidence rate ratio/IRR 3,39 (IK 95% 1,43–8,04); IRR 2,36 (IK 95% 1,08–5,17); dan IRR 4,08 (IK 95% 1,78–9,34)). Nilai IRR aberans CD19 dan t(8;21) IRR < 1.Penelitian ini menunjukkan aberans CD7, inv(16) dan mutasi FLT3-ITD dapat dijadikan faktor prognosis baik sedangkan aberans CD19, kariotipe t(8;21) dapat dijadikan faktor prognosis buruk pada LMA anak di Indonesia.

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Currently, pediatric acute myeloid leukemia (AML) patients who achieved complete remission after induction therapy has reach only 49% with 10% event-free survival (EFS) rate. The relapse rate and mortality related to chemotherapy are the causes of this low outcome. To improve outcomes and reduce side effects of treatment, it is necessary to carry out risk stratification using cytogenetic profiles and immunophenotypes. The purpose of this study was to obtain profiles of immunophenotype, karyotype, FLT3-ITD and NPM1 mutations (prognostic variables), and their relationship to the response to induction chemotherapy.

The study was conducted with an analytical cohort design on AML patients aged 1–18 years at RSCM, RSABHK, RSKAD, RSPAD from November 2018 to March 2020. The examinations included expression of CD7, CD19, karyotype t(8.21), inv(16), NPM1 and FLT3-ITD mutations, then assessed the relationship with the incidence of remission after receiving induction therapy with the National AML protocol.

Of the 42 subjects, the median age was 8 years 11 months (3–213 months). The most common type of AML was M1, followed by M2. The most common clinical symptoms were pallor (33/42) and fever (25/42). The most common clinical signs were hepatomegaly (17/42) and splenomegaly (18/42). Subjects with CD7+ 21.4%, CD19+ 11.9%. Translocation t(8;21) was detected in 1 of 18 (5.6%) subjects, inv(16) in 4 of 18 ((22%) subjects, 7 of 18 subjects included in the favorable karyotype group. A total of 2 of 28 (7%) subjects had FLT3-ITD mutations. NPM1 mutation was not found. Role of CD7 expression as prognostic factor was more dominant than age and leukocyte count at diagnosis. Multivariate analysis using generalized linear model showed a significant relationship between prognostic variables and response to induction therapy. CD7 aberrant, inv(16) and FLT3-ITD mutations had a higher relative risk for remission (respectively incidence rate ratio /IRR 3.39 (95% CI 1.43–8.04); IRR 2.36 (95% CI 1.08–5.17); and IRR 4.08 (95% CI 1.78–9.34)). Incidence rate ratio value of CD19 aberrant and t(8;21) IRR < 1.

This study showed that CD7 aberrant, inv(16) and FLT3-ITD mutations can be used as good prognostic factors, while CD19 aberrant, t(8;21) karyotype can be used as poor prognostic factors for pediatric AML in Indonesia."

"Latar Belakang: Respons imun berperan pada kerentanan pasien talasemia terhadap infeksi. Defisiensi seng pada talasemia akan memperburuk respons imun. Penelitian ini bertujuan mengetahui profil respons imun pasien talasemia mayor dan pengaruh suplementasi seng dan imunisasi pneumokokus pada respons imun pasien talasemia pasca-splenektomi.Metode: Penelitian dilakukan di Pusat Thalassemia RSCM, Jakarta pada September 2013 ? Februari 2014. Studi observasi dengan metode belah lintang komparatif pada talasemia mayor sehat usia > 12 tahun dan HIV negatif non- dan pasca-splenektomi mendahului studi intervensi dengan metode randomized, double-blinded, controlled trial pada talasemia pasca-splenektomi yang dialokasikan menjadi kelompok seng 1,5 mg/kg/hr maksimum 50 mg, atau plasebo. Dua jenis imunisasi pneumokokus diberikan untuk menguji fungsi limfosit T. Luaran yang diukur adalah respons imun non-spesifik (jumlah dan fagositosis neutrofil) dan respons imun spesifik (kuantitatif dan kualitatif). Respons imun spesifik kualitatif mengukur produksi IgG pneumokokus, IL-2 dan TNF-α pasca pajanan PHA.Hasil Penelitian: Median fagositosis neutrofil kelompok pasca-splenektomi 29,79 (4 sampai 81)% dan kelompok non-splenektomi 55,83 (2 sampai 133)% (p < 0,001). Kelompok pasca-splenektomi mempunyai jumlah netrofil, limfosit total, jumlah limfosit T, jumlah limfosit T CD4+ dan CD8+ yang lebih tinggi dibanding kelompok non- splenektomi. Tidak ada perbedaan respons imun spesifik kualitatif yang bermakna di antara pasien talasemia mayor. Setelah intervensi, hanya 18 dari 28 subjek kadar seng serum kelompok seng yang menjadi normal. Walaupun fagositositosis neutrofil hanya berubah dari 31,36 (4 sampai 81)% menjadi 30,44 (3 sampai 72)% (p = 0,554), namun terdapat kecenderungan perbaikan fagositosis neutrofil pada kelompok seng. Parameter respons imun lainnya tidak menunjukkan perubahan antara kelompok seng dan plasebo selama penelitian 12 minggu (p > 0,05).Simpulan: Terdapat perbedaan respons imun antara pasien talasemia pasca-splenektomi dan non-splenektomi. Belum dapat dibuktikan pengaruh suplementasi seng pada hampir semua parameter respons imun pasien talasemia mayor pasca-splenektomi. Seng mungkin dapat direkomendasikan sebagai suplementasi, tetapi perlu penelitian lanjutan mengenai dosis dan lama pemberian yang tepat untuk perbaikan respons imun pasien talasemia mayor pasca-splenektomi.

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Introduction: Immune response plays a role in increasing thalassemia patient?s susceptibility to infections. Zinc deficiency in thalassemia patients will alter immune response. The aim of this study is to evaluate immune response of thalassemia major and zinc supplementation effects on immune response quality of post-splenectomy thalassemia major.

Methods: This study was conducted at Thalassaemia Centre, Cipto Mangunkusumo Hospital Jakarta on September 2013 ? February 2014. An observational study using comparative cross-sectional method was done in healthy non- and post-splenectomy thalassemia major aged > 12 year and HIV negative. Then, it was followed by an interventional study using randomized, double-blinded, controlled trial, on post- splenectomy subjects, which were assigned to receive 1.5 mg/kg/d maximum 50 mg/d zinc or placebo. Moreover, 2 type of immunization were also administered in order to assess T lymphocyte function. The outcomes were non-specific (neutrophil count and phagocytosis) and specific immune response (quantitave and qualitative). Qualitative specific immune response measured by detecting IgG pneumococcal, IL-2 and TNF-α after PHA exposure.

Results: Median of neutrophil phagocytosis on post-splenectomy and non-splenectomy were 29.79 (4 to 81)% and 55.83 (2 to 133)% (p < 0.001). Post-splenectomy subjects have higher neutrophil count, total lymphocyte count, lymphocyte T count, lymphocyte T CD4+ and CD8+ than non-splenectomy. There is no significant difference on qualitative specific immune response among thalassemia major. Following the intervention, only 18 out of 28 subjects of zinc group had normal plasma zinc. There was a trend of neutrophil phagocytosis improvement on zinc group despite a little shifting on those value, from 31.36 (range 4 to 81)% to 30.44 (3 to 72)% (p = 0.554). Other immune response parameters showed no different changes between two groups after 12 weeks supplementation (p > 0.05).

Conclusions: There were significant differences on immune response of post- splenectomy and non-splenectomy patients. The significant changes on almost all of immune response parameter after zinc supplementation have not been proved yet. Addition of zinc supplementation may be recommended, but it need further study to evaluate the dose and duration of supplementation to improve immune response in splenectomised thalassemia major patients."

"Latar Belakang: Di Indonesia diperkirakan terdapat 4100 kasus baru kanker anak setiap tahunnya. Kejadian paling banyak adalah leukemia limfoblastik akut LLA sebesar 80 . Permasalahannya adalah angka kejadian kekambuhan pasien anak cukup tinggi sekitar 20-40 . Data pasien anak di Bagian Hematologi/Onkologi Departemen Ilmu Kesehatan Anak RSCM/FKUI periode tahun 2005-2011 kejadian kambuh mencapai 40 . Tujuan penelitian ini adalah mengetahui apakah ada hubungan kekambuhan pasien anak LLA terkait terapi vinkristin dengan polimorfisme gen MDR1.Metode: Studi dilakukan di Departemen Ilmu Kesehatan Anak RSCM/FKUI selama periode Februari 2014 sampai Januari 2015 dengan disain penelitian cohort. Kriteria pasien dengan LLA berusia lebih dari satu tahun hingga usia kurang dari 18 tahun. Sampel adalah pasien baru didiagnosis LLA dan pasien sedang menjalani kemoterapi fase induksi. Pemeriksaan sensitifitas obat in vitro dari sampel darah metode flow cytometry dengan menghitung Leukemia Cell Survival Index LCSI . Penelitian pendahuluan gen MDR1 dengan RFLP dan polimorfisme dengan Multiplex PCR. Data klinis pasien dilihat secara retrospektif dari catatan medis. Inform consent diperoleh dari pasien atau orang tua pasien.Hasil: Sampel memenuhi kriteria inklusi sebanyak 101 pasien terdiri dari 63 62.4 laki-laki dan 38 37.6 perempuan. Kekambuhan pasien anak LLA dipengaruhi oleh faktor usia,kelompok risiko dan jumlah lekosit p

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Background There are an estimated 4100 new cases of childhood cancer each year in Indonesia. The most common cancer in children is acute lymphoblastic leukemia ALL which is approximately 80 . The problem faced is the incidence of relapse in children is quite high, about 20 40 . Data from Hematology Oncology Division of Child Health Department RSCM FKUI period 2005 2011, showed that the incidence of relapse reached 40 . The purpose of this study is to investigate whether there is an association of polymorphism related to vincristine therapy.Methods The study was conducted in the Child Health Department RSCM FKUI with cohort design from February 2014 to January 2015. The number of patients with ALL included in the study was 101. The patients participated in the study were 1 18 years old, newly diagnosed of ALL, and undergoing chemotherapy induction phase. In vitro examination of drug sensitivity from blood samples was conducted using flow cytometry to determine leukemia cell survival index LCSI . The preliminary study was done by RFLP and polymorphism by Multiplex PCR. Clinical data of patients were obtained retrospectively from medical records.The informed consent was obtained from the patient or the patient 39 s parents.Results From 101 patients, there were 63 male 62.4 and 38 female 37.6 . The occurence of relapse of ALL patients was affected by age, risk group and leukocyte count p"

"Akumulasi rantai globin-α berlebihan pada membran SDM thalassemia-β mayor menyebabkan hemolisis, eritropoiesis tidak efektif dan anemia kronik sehingga memerlukan transfusi sel darah merah (SDM) terus menerus. Transfusi rutin dan hemolisis mengakibatkan besi bebas sebagai radikal bebas dan membentuk radikal peroksil lipid di membran SDM sehingga memperberat hemolisis. Antioksidan α-tokoferol menghambat pembentukan radikal peroksil lipid tersebut.Penelitian ini bertujuan untuk menilai peran α-tokoferol terhadap hemolisis dan stres oksidatif. Penelitian ini merupakan uji klinis acak tersamar ganda pada thalassemia-β mayor usia 5–18 tahun yang mendapat transfusi dan kelasi besi rutin di Pusat Thalassemia RSUP dr.Ciptomangunkusumo Kiara. Intervensi plasebo dan α-tokoferol diberikan selama empat minggu. Suplementasi α-tokoferol berdasarkan rekomendasi Institute of Medicine (IOM), 4–8 tahun 200 mg/hari; 9–13 tahun 400 mg/hari; 14–18 tahun 600 mg/hari. Penilaian penanda hemolisis menggunakan haptogobin (Hp), hemopeksin (Hx) dan fragilitas osmotik SDM. Penanda stres oksidatif yaitu MDA, GSH, GSSG, rasio GSH/GSSG dan α-tokoferol. Pemeriksaan laboratorium dilakukan sebelum dan setelah diberikan plasebo/α-tokoferol, sesaat sebelum transfusi SDM. Analisis uji t-tidak berpasangan untuk melihat perbedaan antara kelompok studi dan uji korelasi untuk melihat hubungan antara variabel.Pada bulan Desember 2016 hingga Juli 2017, 40 subjek mampu menyelesaikan penelitian, 20 subjek kelompok plasebo dan 20 subjek kelompok α-tokoferol. Nilai rerata Hp lebih besar pada kelompok α-tokoferol (3,01 mg/dL) dibandingkan kelompok plasebo (1,08 mg/dL), secara statistik berbeda bermakna (p = 0,021). Nilai rerata kadar Hx dan persentase hemolisis SDM tidak berbeda bermakna pada kedua kelompok studi (p > 0,05). Tidak ada perbedaan bermakna pada kelompok α-tokoferol dan plasebo untuk kadar MDA (1,003 nmol/L dan 1,07 nmol/L), GSH (5,81 µM dan 6,15 µM), GSSG (1,77 µM dan 1,86 µM) dan rasio GSH/GSSG (1,29 dan 1,31), (P > 0,05).Antioksidan α-tokoferol dapat mengurangi hemolisis dan secara tidak langsung memperbaiki kadar Hp pada thalassemia-β mayor, akan tetapi tidak mampu memengaruhi stres oksidatif.

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The accumulation of excess unmatchedα-globin chains in the red blood cell membrane of β-thalassemia major leads to hemolysis, ineffective erythropoiesis and chronic anemia which needs multiple red blood cell transfusion. Routine transfusions may lead to iron overload as free radical in the red blood cell membrane, resulting clinically as severe hemolysis. Alpha-tocopherol as an antioxidant has been known as a potent scavenger of hydroxyl lipid radical.The aim of this study was to evaluate the effects of α-tocopherol in hemolysis and oxidative stress on the red cell membrane in β-thalassemia major. This randomized double-blind, placebo-controlled study was done in β-thalassemia major patients range aged 5–18 years old who regularly had transfusion and receiving iron chelating agents at Thalassemia centre, Kiara Ciptomangunkusumo Hospital. All subjects were randomized to receive either α-tocopherol or placebo orally for 4 weeks. Subjects in the experimental group received α-tocopherol, the doses based on the recommendation from Institute of Medicine (IOM) as follows: 200 mg/day for 4–8 years old; 400 mg/day for 9–13 years old; 600 mg/day for 14–18 years old. Laboratory analysis for hemolysis variables were haptoglobin, hemopexin, osmotic fragility test. Oxidative stress and antioxidant variables were MDA, GSH, GSSG, GSH/GSSG ratio, and α-tocopherol. All variable were evaluated before 4 weeks and after consuming α-tocopherol or placebo, just before they received a blood transfusion. The statistical analysis results using independent t-test and correlation test.During December 2016–July 2017, 40 subjects completed the study, they were 20 subjects in the placebo group and 20 subjects in the α-tocopherol group. There was significant enhancement of haptoglobin mean level in the α-tocopherol group (3.01 mg/dL) compared to placebo (1.08 mg/dL), (p = 0.021). The mean level of hemopexin and the percentage of RBC hemolysis did not significantly different in both groups, (p > 0.05). We also did not find any significantly different in mean level of MDA (1.003 nmol/L and 1.07 nmol/L), GSH (5.81 µM and 6.15 µM), GSSG (1.77 µM and 1.86 µM) and GSH/GSSG ratio (1.29 and 1.31), (p > 0.05) for the α-tocopherol and placebo groups.The effects of α-tocopherol may improve hemolysis and haptoglobin level indirectly in β-thalassemia major, but there was no significant role in oxidative stress."

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ABSTRAK

 

Nama                        : Saptuti Chunaeni

Program Studi             : Program Doktor Ilmu Biomedik

Judul Disertasi             : Upaya Meningkatan Stabilitas Faktor VIII melalui

  Liofilisasi Produk Minipool Cryoprecipitate

  untuk Tatalaksana Penderita Hemofilia A di Indonesia.

Latar Belakang: Penderita Hemofilia di Indonesia sekitar 2.000 orang tersebar dari Sabang hingga Merauke. Di Jabodetabek, 403 anak penderita hemofilia, 86% hemofilia A dan 54% diantaranya hemofilia A berat. Konsentrat F VIII digunakan untuk terapi sulih Hemofilia A, mahal, harus impor dan tidak selalu tersedia. Kriopresipitat sebagai terapi sulih alternatif, kandungan F VIII sedikit dan pemberiannya untuk segolongan darah. MC cair dari Mesir, dapat meningkatkan kandungan dan keamanan F VIII. Bentuknya cair dan suhu penyimpanan minus 30°C, sehingga perlu ditingkatkan stabilitasnya dengan liofilisasi menjadi MC kering.

Tujuan:Tujuan penelitian ini adalah untuk mengetahui stabilitas dan keamanan MC kering lebih besar atau sama dengan MC cair.

Metode:Liofilisasi MC cair menjadi MC kering dilakukan agar lebih stabil dan dapat disimpan di suhu dingin (2-6°C) dan suhu ruang ( > 25°C). MC kering, ada yang ditambah eksipien (KE+) dan tanpa eksipien (KE-). Dilakukan uji banding stabilitas MC cair dan MC kering pada hari ke 0, 7, 30 dan 240, meliputi pemeriksaan kandungan F VIII, pH, osmolalitas dan kelarutan. Pemeriksaan keamanan MC cair menggunakan flowcytometri dan MC kering dengan hemaglutinasi dan kontaminasi bakteri.  

Hasil:MC Kering tanpa Eksipien (KE-) pada waktu penyimpanan 30 hari (T₃₀) lebih tinggi F VIII-nya dibandingkan MC Kering dengan Eksipien (KE+) dan MC Cair. Namun pada waktu penyimpanan 240 hari (T₂₄₀) penurunan F VIII pada KE- lebih banyak daripada KE+. Keamanan dengan memeriksa kontaminasi bakteri dan hemaglutinin pada MC kering sama dengan MC cair. 

Kesimpulan:MC kering tanpa eksipen yang disimpan pada suhu dingin dan suhu kamar, stabilitas kandungan F VIII sangat baik pada hari ke 30. Penambahan eksipien yang terlalu banyak, dapat menghancurkan protein yang terkandung di dalamnya. Keamanan MC kering sama dengan MC cair.

Kata kunci: F VIII, Hemofilia A, MC kering, Stabilitas.

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ABSTRACT

 

Name                           : Saptuti Chunaeni

Programme of study   :Doctoral Program in Biomedical Science

Title                             :To Improve Stability of Factor VIII with Minipool

 Cryoprecipitate Lyophilized for Hemofilia a Treatment in

 Indonesia

 

 

Background:  There are about 2.000 hemophilia patients in Indonesia. Nowadays in

Jabodetabek alone, there are 403 children hemophilia mostly of 86% hemophilia A and 54% among them are of severe type.

Use of F VIII concetrate as a standard replacement therapy of hemophilia A, is expensive, needs to be imported from overseas and it is not always available. Cryoprecipitate as an alternative replacement therapy contains only a small yield F VIII and is only available for same blood group patients. Liquid minipool cryoprecipitate (MC) from Egypt can increase the F VIII content and safety. The MC, however is liquid and must be stored at – 30^oC. Considering this, there is a need to improve the stability of F VIII by lyophilization procedure.

The aim of present study was to determine whether the stability and safety of dry MC was greater or equal to liquid MC.

Materials and Methods:Liquid of MC was lyophilized and was added excipients (KE+) or without excipient (KE-). Liyophilization is carried out to be more stable and can be stored at cold temperatures and room temperature. Tests on the stability on certain days (0, 7, 30 and 240.) including examination of F VIII content, pH, osmolality and solubility. Safety checks using flowcytometry and hemagglutination and bacterial contamination.

Results: Dry MC at T30 was higher in F VIII. At storage T240 the decrease in F VIII at KE- was more than KE +. The safety of a dry MC is the same as a liquid MC.

Conclusion: F VIII at KE- is better on T30. Adding excipients can destroy protein. The safety is the same.

Keywords:  F VIII, Hemophilia A, Lyophilized MC, Stability.

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