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"ABSTRAKLimfoma malignum ialah suatu penyakit keganasan primer daripada jaringan limfoid yang bersifat padat. Penyakit ini dibagi dalam dua golongan besar, yaitu penyakit Hodgkin dan limfoma non-Hodgkin (LNH). Sel ganas pada penyakit Hodgkin berasal dart sel retikulum. Limfosit-limfosit yang merupakan bagian integral proliferasi sel pada penyakit ini diduga merupakan manifestasi reaksi kekebalan seluler terhadap sel-sel ganas tadi. Limfoma non-Hodgkin pada dasarnya merupakan keganasan sel limfosit.Pada penyakit Hodgkin telah dicapai kesepakatan mengenai prosedur diagnostik yang harus dilakukan untuk menetapkan diagnosis, tingkat penyakit dan mengenai pengobatan penderita. Pada LNH keadaannya amat berbeda. Hal ini tercermin pada usaha terus menerus selama seperempat abad ini untuk mengajukan penggolongan-penggolongan dan nomenklatur-nomenklatur yang baru. Di samping itu skema yang tetap untuk menilai tingkat penyakit maupun pengobatan belum ada.1. Gambaran umum penderita-penderita INH di JakartaSelama lima tahun terakhir, yaitu antara tanggal 1 Oktober 1978 hingga 1 Oktober 1983, 583 penderita baru limfoma malignum dijumpai di Subbagian Hematologi Bagian Ilmu Penyakit Dalam, Rumah Sakit Dr. Cipto Mangunkusumo, Fakultas Kedokteran Universitas Indonesia. Penilaian histologis jaringan tumor penderita-penderita tersebut dibuat oleh ahli Patologi Anatomik berbagai laboratorium di Jakarta dan di luar Jakarta, 88,5% di antaranya didiagnosis sebagai LNH.Duaratus tujuh puluh lima di antara 583 penderita baru tersebut datang antara tanggal 1 Oktober 1978 hingga I April 1981 dan diteliti lebih lanjut. Diagnosis histologis pada 250 penderita dibuat oleh ahli Patologi Anatomik Fakultas Kedokteran Universitas Indonesia. Duabelas kasus telah diperiksa di rumah sakit lain, namun diagnosis histologisnya diteliti kembali oleh bagian Patologi Anatomik Fakultas Kedokteran Universitas Indonesia. Pada tigabelas kasus lainnya, diagnosis dibuat oleh ahli Patologi Anatomik dari laboratorium lain. Di antara 275 penderita ini, hanya 30 orang (10,9(1o) yang menderita penyakit Hodgkin sedangkan 245 orang menderita penyakit LNH (89,1 %).Angka kejadian penyaldt Hodgkin yang rendah telah dilaporkan oleh Soeripto (211) yang menemukan hanya dua orang penderita (2,607o) penyakit Hodgkin di antara 75 penderita limfoma malignum yang ditelitinya. Angka-angka yang rendah juga ditemukan di Irian Timur (Papua New Guinea) dan Jepang (tabel 1). Penyebab variasi geografis ini tidak diketahui walaupun bukti-bukti yang ada pada waktu ini menunjukkan bahwa berbagai faktor yang berhubungan dengan "tuan rumah" dan lingkungan turut berperan.2. Tujan penelitianLNH ialah suatu penyakit yang heterogen. Bergantung pada gambaran his tologis tumomya, perjalanan penyaldt penderita dapat bermacam-macam mulai dari yang perkembangannya amat lambat dan dapat disandang dengan baik sampai pada yang cepat berkembang menjadi fatal. Penderita-penderita penyakit LNH derajat keganasan rendah acapkali tidak memerlukan pengobatan selama bertahun-tahun, namun penyembuhan yang sempuma jarang terjadi. Sebaliknya beberapa kelompok dengan penyakit yang cepat menjadi fatal bila tidak diobati, mempunyai harapan untuk sembuh jika mendapat pengobatan yang tepat.Selain bergantung pada gambaran histologis tumor, pengobatan LNH bergantung juga pada tingkat penyakit penderita. Hingga saat ini belum ada keseragaman mengenai pemeriksaan-pemeriksaan yang dilakukan dalam penatalaksanaan penderita penyakit LNH. Di negaranegara maju acapkali dilakukan berbagai pemeriksaan yang rumit dan mahal untuk dapat memperoleh keterangan yang lengkap mengenai penyakit penderita. Selain biaya pemeriksaannya, biaya pengobatan penyakit LNH juga sangat mahal, sedangkan hasil yang dicapai acapkali mengecewakan. Memperpanjang masa harapan hidup penderita dengan beberapa bulan mungkin penting artinya dalam rangkaian up coba klinis untuk perbaikan pengobatan penderita di masa depan, tetapi agaknya tidak relevan untuk negara yang mempunyai keterbatasan dana seperti di Indonesia.Penelitian ini bertujuan untuk mengenal pola penyakit LNH di Indonesia (meliputi aspek histologis, sitologis, imunologis dan klinis) serta menentukan strategi yang paling berdaya guna dan tepat guna dalam menetapkan diagnosis, tingkat penyaldt dan pengobatan penyakit LNH di negara ini, dengan mempertimbangkan hambatan segi kedokteran maupun ekonomi yang terdapat di sini."

"Latar belakang:Kondisi hiperglikemia pada diabetes melitus (DM) yang tidak terkontrol dan berlangsung lama dapat menimbulkan dampak negatif. Salah satu konsekuensi dari DM adalah munculnya penyakit arteri perifer (PAP) dan neuropati perifer diabetik (NPD). NPD merupakan komplikasi diabetes yang menunjukkan tanda dan gejala gangguan motorik dan sensorik, sementara PAP adalah kondisi aterosklerosis yang berkembang perlahan pada pembuluh arteri. Kedua penyakit ini menunjukkan gejala kelainan motorik dan sensorik yang saling tumpang tindih.Tujuan:Penelitian ini bertujuan untuk mengetahui hubungan stenosis arteri yang dinilai menggunakan arteriografi terhadap gangguan saraf yang dinilai menggunakan pemeriksaan kecepatan hantar saraf (KHS) pada pasien DM tipe 2 dengan PAP dan NPD.Metode:Penelitian ini merupakan penelitian potong lintang yang mengambil data sekunder dari data penelitian sebelumnya yang dilakukan pada Juli 2018 hingga Juni 2021 RSUPN Cipto Mangunkusumo. Subjek penelitian ini adalah penyandang DM yang memiliki NPD dan PAP yang memenuhi kriteria inklusi dan tidak memenuhi kriteria eksklusi. Subjek penelitian kemudian menjalani pemeriksaan arteriografi untuk menilai stenosis pada A. Peroneal, A. Tibialis Anterior dan A. Tibialis Posterior. Subjek penelitian juga menjalani pemeriksaan kecepatan hantar saraf (KHS) pada N. Peroneal Communis, N. Peroneal Superficialis, N. Tibialis dan N. Suralis. Korelasi antar kedua variabel kemudian diuji dengan Uji Korelasi Spearman.Hasil:Hasil menunjukkan bahwa stenosis A. Peroneal memiliki korelasi negatif derajat sedang (r = - 0.420) dengan KHS sensorik N. Peroneal Superficialis yang bermakna secara statistik (p = 0.023). Sementara itu, hubungan stenosis dan gangguan KHS pada A. Peroneal dengan N. Peroneal Communis, A. Tibialis Anterior dengan N. Tibialis dan A. Tibialis Posterior dengan N. Suralis memiliki korelasi yang tidak bermakna secara statistik (p >0.05). Hal ini dapat dijelaskan oleh kemungkinan kolateral yang dapat muncul pada penyandang PAP, struktur anatomi vaskular terhadap syaraf, dan jumlah sampel yang kecil.Kesimpulan:Terdapat korelasi negatif derajat sedang antara derajat stenosis A. Peroneal dan KHS sensorik N. Peroneal Superficialis. Namun hasil yang tidak bermakna ditemukan pada hubungan A. Peroneal dengan N. Peroneal Communis, A. Tibialis Anterior dengan N. Tibialis dan A. Tibialis Posterior dengan N. Suralis.

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Background:

The condition of hyperglycemia in uncontrolled and prolonged diabetes mellitus (DM) can have negative impacts. One consequence of DM is the emergence of peripheral artery disease (PAD) and diabetic peripheral neuropathy (DPN). DPN is a complication of diabetes that presents signs and symptoms of motor and sensory disturbances, while PAD is an atherosclerosis condition that gradually develops in the arterial vessels. Both diseases exhibit overlapping symptoms of motor and sensory abnormalities.

Objective:

This study aims to determine the correlation of arterial obstruction assessed using arteriography and the nerve impairment assessed using nerve conduction velocity (NCV) in DM patients with PAD and DPN.

Methods:

This is a cross-sectional study that takes secondary data from previous research data conducted from July 2018 to June 2021 RSUPN Cipto Mangunkusumo. The subjects of this study were people with DM who had NPD and PAP who met the inclusion criteria and did not meet the exclusion criteria. The research subjects then underwent an arteriography examination to assess the stenosis in the peroneal artery, anterior tibial artery and posterior tibial artery. Research subjects also underwent nerve conduction velocity (KHS) examinations in the Peroneal N. Communis, N. Peroneal Superficialis, N. Tibialis and N. Suralis. The correlation between the two variables was then tested using the Spearman Correlation Test.

Results:

The results showed that the Peroneal Artery stenosis had a moderate negative correlation (r = - 0.420) with the sensory NCV of the Superficial Peroneal Nerve which was statistically significant (p = 0.023). Meanwhile, the correlation of stenosis and NCV disorders in the Peroneal Nerve with the Common Peroneal Nerve, Anterior Tibial Nerve with Tibialis Nerve and Posterior Tibial Nerve with Sural Nerve had a correlation that was not statistically significant (p > 0.05). This can be explained by the possibility of collaterals appearing in people with PAD, the structure of vasculature on the nerves, and the small number of samples.

Conclusion:

There is a moderate negative correlation between the degree of stenosis of the Peroneal nerve and the sensory NCV of the Peroneal Superficialis. However, insignificant results were found in the correlation between Peroneal Artery with Common Peroneal Nerve, Anterior Tibialis Artery with Tibial Nerve and Posterior Tibial Artery with Sural Nerve."

"[ABSTRAKHipoksia berperan penting pada patofisiologi berbagai penyakit utama penyebab kematian seperti, penyakit jantung iskemia, strok, kanker, penyakit paru kronik, dan gagal jantung kongestif. Kedua protein golongan globin di otak, yaitu neuroglobin (Ngb) dan sitoglobin (Cygb) diduga berperan dalam suplai oksigen ke mitokondria dan melindungi jaringan otak dari kerusakan akibat hipoksia (neuroprotektan). Perubahan ekspresi protein merupakan salah satu bentuk adaptasi biokimia yang penting terhadap perubahan homeostasis. Oleh karena itu timbul pertanyaan bagaimana pola ekspresi Ngb dan Cygb serta peran neuroprotektan kedua protein tersebut di otak pada keadaan hipoksia sistemik kronik (HSK). Penelitian bertujuan manganalisis perbedaan pola ekspresi Ngb dan Cygb serta kaitannya dengan apoptosis pada HSK. Parameter yang diukur adalah Ngb, Cygb, sitokrom c, MDA, GSH dan HIF-lα. Rancangan penelitian yang digunakan adalah studi eksperimental in vivo model HSK pada tikus. Tikus sebagai hewan coba dibagi secara acak dalam 6 kelompok perlakuan, yaitu kelompok I adalah kelompok kontrol atau tanpa perlakuan hipoksia, sedangkan kelompok II, III, IV, V, dan VI mendapat perlakuan hipoksia dengan lama waktu hipoksia selama 1, 3, 5, 7, dan 14 hari. Parameter yang diperiksa meliputi ekspresi Ngb dan Cygb dengan teknik real time-RT PCR, ELISA dan imunofluoresen FITC, stres oksidatif, HIF-1α sebagai penanda hipoksia, dan sitokrom c sebagai penanda apoptosis. Hasil yang diperoleh HSK meningkatkan ekspresi mRNA Ngb pada hipoksia 3, 5, dan 7 hari, namun ekspresi proteinnya menurun pada hipoksia 1, 3, 5, 7, dan 14 hari dibanding dengan kontrol. Berbeda dengan ekspresi mRNA Cygb yang menurun selama hipoksia 1, 3, 5, 7, dan 14 hari, namun protein Cygb meningkat pada hipoksia 1, 3, 5, 7, dan 14 hari dibandingkan dengan kontrol. Korelasi Ngb dengan sitokrom c lemah tidak signifikan, sedangkan Cygb sangat lemah dan tidak signifikan. HSK menginduksi ekspresi HIF-lα yang meningkat tertinggi pada hipoksia 7 hari, dan menyebabkan stres oksidatif yang ditandai dengan meningkatnya MDA pada hipoksia 1, 3 dan 5 hari, serta menurunnya GSH pada hipoksia 1, 3, dan 5 hari. Penelitian ini membuktikan bahwa terdapat perbedaan pola ekspresi Ngb dan Cygb pada HSK. Ekspresi Ngb sebagai respons adaptasi terjadi lebih awal dan lebih dipengaruhi oleh lama waktu hipoksia dibandingkan dengan ekspresi Cygb. Meskipun lemah, Ngb cenderung mempunyai peran menghambat apoptosis dibandingkan dengan protein Cygb.;

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ABSTRACTHypoxia has an important role in the pathophysiology of high mortality diseases, such as ischemic cardiovascular disease, stroke, cancer, chronic lung disease, and congestive heart failure. The proteins belonged to globin protein group, included neuroglobin (Ngb) and cytoglobin (Cygb), have been presumed to play a role in regulating the oxygen supply into the mitochondria and protecting the brain tissues from damage due to hypoxia (neuroprotectant). An alteration in protein expression due to a homeostatic shift is an important adaptation process in biochemistry. Therefore, the expression pattern of Ngb and Cygb as well as their protein roles in brain during a chronic systemic hypoxia condition (CSH) remain unclear. This study aim to analyse the differences of the Ngb and Cygb expression patterns, and correlation of both protein to apoptosis in chronic systemic hypoxic condition. Ngb, Cygb, Cytochrome c, MDA, GSH, and HIF-1 α. were examined. An in vivo experimental model of CSH was carried out using rat. The experimental rats were randomly divided into 6 treatment groups, i.e. group I was a control group or without hypoxic condition, groups II, III, IV, V, and VI were treated by hypoxic condition for 1, 3, 5, 7, and 14 days, respectively. The Ngb and Cygb expressions were analysed using real time-RTPCR, ELISA, immunofluorescence with FITC, and the measurement of stress oxidative biomarkers, included HIF-1α as a biomarker of hypoxic condition and cytochrome c as a biomarker of apoptosis. The CSH was increased the mRNA expression of Ngb at 3, 5, and 7 days hypoxic groups, while the protein expression was decreased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The mRNA expression of Cygb was decreased at 1, 3, 5, 7, and 14 days hypoxic groups, whereas the Cygb protein expression was increased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The correlation between Ngb with cytochrome c was weakly statistically insignificant, and Cygb with cytochrome c was statistically insignificant. The CSH induced the HIFlα, which was shown by a high increase at 7 days hypoxic group, as well as stress oxidative which was represented by MDA at 1, 3, and 5 days hypoxic groups, and decreased GSH at 1, 3, and 5 days hypoxic groups. There are differences in expression pattern of Ngb and Cygb in CSH. The expression of Ngb, as an adaptive response, occurs earlier and is more influenced by the duration of hypoxic condition compared to Cygb. Although the correlation is weak, the Ngb seems more likely to inhibit apoptosis compared to Cygb protein;Hypoxia has an important role in the pathophysiology of high mortality diseases, such as ischemic cardiovascular disease, stroke, cancer, chronic lung disease, and congestive heart failure. The proteins belonged to globin protein group, included neuroglobin (Ngb) and cytoglobin (Cygb), have been presumed to play a role in regulating the oxygen supply into the mitochondria and protecting the brain tissues from damage due to hypoxia (neuroprotectant). An alteration in protein expression due to a homeostatic shift is an important adaptation process in biochemistry. Therefore, the expression pattern of Ngb and Cygb as well as their protein roles in brain during a chronic systemic hypoxia condition (CSH) remain unclear. This study aim to analyse the differences of the Ngb and Cygb expression patterns, and correlation of both protein to apoptosis in chronic systemic hypoxic condition. Ngb, Cygb, Cytochrome c, MDA, GSH, and HIF-1 α. were examined. An in vivo experimental model of CSH was carried out using rat. The experimental rats were randomly divided into 6 treatment groups, i.e. group I was a control group or without hypoxic condition, groups II, III, IV, V, and VI were treated by hypoxic condition for 1, 3, 5, 7, and 14 days, respectively. The Ngb and Cygb expressions were analysed using real time-RTPCR, ELISA, immunofluorescence with FITC, and the measurement of stress oxidative biomarkers, included HIF-1α as a biomarker of hypoxic condition and cytochrome c as a biomarker of apoptosis. The CSH was increased the mRNA expression of Ngb at 3, 5, and 7 days hypoxic groups, while the protein expression was decreased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The mRNA expression of Cygb was decreased at 1, 3, 5, 7, and 14 days hypoxic groups, whereas the Cygb protein expression was increased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The correlation between Ngb with cytochrome c was weakly statistically insignificant, and Cygb with cytochrome c was statistically insignificant. The CSH induced the HIFlα, which was shown by a high increase at 7 days hypoxic group, as well as stress oxidative which was represented by MDA at 1, 3, and 5 days hypoxic groups, and decreased GSH at 1, 3, and 5 days hypoxic groups. There are differences in expression pattern of Ngb and Cygb in CSH. The expression of Ngb, as an adaptive response, occurs earlier and is more influenced by the duration of hypoxic condition compared to Cygb. Although the correlation is weak, the Ngb seems more likely to inhibit apoptosis compared to Cygb protein;Hypoxia has an important role in the pathophysiology of high mortality diseases, such as ischemic cardiovascular disease, stroke, cancer, chronic lung disease, and congestive heart failure. The proteins belonged to globin protein group, included neuroglobin (Ngb) and cytoglobin (Cygb), have been presumed to play a role in regulating the oxygen supply into the mitochondria and protecting the brain tissues from damage due to hypoxia (neuroprotectant). An alteration in protein expression due to a homeostatic shift is an important adaptation process in biochemistry. Therefore, the expression pattern of Ngb and Cygb as well as their protein roles in brain during a chronic systemic hypoxia condition (CSH) remain unclear. This study aim to analyse the differences of the Ngb and Cygb expression patterns, and correlation of both protein to apoptosis in chronic systemic hypoxic condition. Ngb, Cygb, Cytochrome c, MDA, GSH, and HIF-1 α. were examined. An in vivo experimental model of CSH was carried out using rat. The experimental rats were randomly divided into 6 treatment groups, i.e. group I was a control group or without hypoxic condition, groups II, III, IV, V, and VI were treated by hypoxic condition for 1, 3, 5, 7, and 14 days, respectively. The Ngb and Cygb expressions were analysed using real time-RTPCR, ELISA, immunofluorescence with FITC, and the measurement of stress oxidative biomarkers, included HIF-1α as a biomarker of hypoxic condition and cytochrome c as a biomarker of apoptosis. The CSH was increased the mRNA expression of Ngb at 3, 5, and 7 days hypoxic groups, while the protein expression was decreased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The mRNA expression of Cygb was decreased at 1, 3, 5, 7, and 14 days hypoxic groups, whereas the Cygb protein expression was increased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The correlation between Ngb with cytochrome c was weakly statistically insignificant, and Cygb with cytochrome c was statistically insignificant. The CSH induced the HIFlα, which was shown by a high increase at 7 days hypoxic group, as well as stress oxidative which was represented by MDA at 1, 3, and 5 days hypoxic groups, and decreased GSH at 1, 3, and 5 days hypoxic groups. There are differences in expression pattern of Ngb and Cygb in CSH. The expression of Ngb, as an adaptive response, occurs earlier and is more influenced by the duration of hypoxic condition compared to Cygb. Although the correlation is weak, the Ngb seems more likely to inhibit apoptosis compared to Cygb protein;Hypoxia has an important role in the pathophysiology of high mortality diseases, such as ischemic cardiovascular disease, stroke, cancer, chronic lung disease, and congestive heart failure. The proteins belonged to globin protein group, included neuroglobin (Ngb) and cytoglobin (Cygb), have been presumed to play a role in regulating the oxygen supply into the mitochondria and protecting the brain tissues from damage due to hypoxia (neuroprotectant). An alteration in protein expression due to a homeostatic shift is an important adaptation process in biochemistry. Therefore, the expression pattern of Ngb and Cygb as well as their protein roles in brain during a chronic systemic hypoxia condition (CSH) remain unclear. This study aim to analyse the differences of the Ngb and Cygb expression patterns, and correlation of both protein to apoptosis in chronic systemic hypoxic condition. Ngb, Cygb, Cytochrome c, MDA, GSH, and HIF-1 α. were examined. An in vivo experimental model of CSH was carried out using rat. The experimental rats were randomly divided into 6 treatment groups, i.e. group I was a control group or without hypoxic condition, groups II, III, IV, V, and VI were treated by hypoxic condition for 1, 3, 5, 7, and 14 days, respectively. The Ngb and Cygb expressions were analysed using real time-RTPCR, ELISA, immunofluorescence with FITC, and the measurement of stress oxidative biomarkers, included HIF-1α as a biomarker of hypoxic condition and cytochrome c as a biomarker of apoptosis. The CSH was increased the mRNA expression of Ngb at 3, 5, and 7 days hypoxic groups, while the protein expression was decreased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The mRNA expression of Cygb was decreased at 1, 3, 5, 7, and 14 days hypoxic groups, whereas the Cygb protein expression was increased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The correlation between Ngb with cytochrome c was weakly statistically insignificant, and Cygb with cytochrome c was statistically insignificant. The CSH induced the HIFlα, which was shown by a high increase at 7 days hypoxic group, as well as stress oxidative which was represented by MDA at 1, 3, and 5 days hypoxic groups, and decreased GSH at 1, 3, and 5 days hypoxic groups. There are differences in expression pattern of Ngb and Cygb in CSH. The expression of Ngb, as an adaptive response, occurs earlier and is more influenced by the duration of hypoxic condition compared to Cygb. Although the correlation is weak, the Ngb seems more likely to inhibit apoptosis compared to Cygb protein, Hypoxia has an important role in the pathophysiology of high mortality diseases, such as ischemic cardiovascular disease, stroke, cancer, chronic lung disease, and congestive heart failure. The proteins belonged to globin protein group, included neuroglobin (Ngb) and cytoglobin (Cygb), have been presumed to play a role in regulating the oxygen supply into the mitochondria and protecting the brain tissues from damage due to hypoxia (neuroprotectant). An alteration in protein expression due to a homeostatic shift is an important adaptation process in biochemistry. Therefore, the expression pattern of Ngb and Cygb as well as their protein roles in brain during a chronic systemic hypoxia condition (CSH) remain unclear. This study aim to analyse the differences of the Ngb and Cygb expression patterns, and correlation of both protein to apoptosis in chronic systemic hypoxic condition. Ngb, Cygb, Cytochrome c, MDA, GSH, and HIF-1 α. were examined. An in vivo experimental model of CSH was carried out using rat. The experimental rats were randomly divided into 6 treatment groups, i.e. group I was a control group or without hypoxic condition, groups II, III, IV, V, and VI were treated by hypoxic condition for 1, 3, 5, 7, and 14 days, respectively. The Ngb and Cygb expressions were analysed using real time-RTPCR, ELISA, immunofluorescence with FITC, and the measurement of stress oxidative biomarkers, included HIF-1α as a biomarker of hypoxic condition and cytochrome c as a biomarker of apoptosis. The CSH was increased the mRNA expression of Ngb at 3, 5, and 7 days hypoxic groups, while the protein expression was decreased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The mRNA expression of Cygb was decreased at 1, 3, 5, 7, and 14 days hypoxic groups, whereas the Cygb protein expression was increased at 1, 3, 5, 7, and 14 days hypoxic groups compared to control group. The correlation between Ngb with cytochrome c was weakly statistically insignificant, and Cygb with cytochrome c was statistically insignificant. The CSH induced the HIFlα, which was shown by a high increase at 7 days hypoxic group, as well as stress oxidative which was represented by MDA at 1, 3, and 5 days hypoxic groups, and decreased GSH at 1, 3, and 5 days hypoxic groups. There are differences in expression pattern of Ngb and Cygb in CSH. The expression of Ngb, as an adaptive response, occurs earlier and is more influenced by the duration of hypoxic condition compared to Cygb. Although the correlation is weak, the Ngb seems more likely to inhibit apoptosis compared to Cygb protein]"

"Circulating tumor cell (CTC) adalah sel tumor yang terlepas dan bersirkulasi di pembuluh darah. Kultur CTC dapat bermanfaat untuk menentukan pengobatan yang efektif dan presisi terhadap penyakit kanker. Akan tetapi, hingga saat ini, kultur CTC masih terbatas dilakukan. Kobalt klorida dilaporkan dapat meningkatkan pertumbuhan sel tumor dalam kultur in-vitro. Namun, kobalt klorida belum pernah digunakan dalam mengultur CTC kanker kolorektal. Oleh karena itu, optimasi konsentrasi CoCl2 dalam mengultur CTC kanker kolorektal penting untuk dilakukan. Parameter yang dapat digunakan dalam optimasi tersebut adalah viabilitas dan jumlah agregasi CTC. Penelitian ini bertujuan untuk mengetahui pengaruh penambahan beberapa konsentrasi CoCl2 (100 dan 150 μM) terhadap viabilitas dan jumlah agregasi CTC kanker kolorektal. Dalam penelitian ini, isolat hasil eritrolisis dikultur dalam medium dengan berbagai konsentrasi CoCl2 (0, 100, dan 150 μM). Kultur kemudian dikonfirmasi dengan immunofluorescence staining menggunakan CK20, PLS3, dan DAPI untuk mengonfirmasi keberadaan CTC kanker kolorektal. Berdasarkan hasil yang diperoleh, ketiga kultur terkonfirmasi mengandung CTC kanker kolorektal. Viabilitas dan jumlah agregasi sel kultur dari yang paling tinggi ke paling rendah teramati pada perlakuan 0, 100, dan 150 μM CoCl2. Berdasarkan penelitian ini, dapat disimpulkan bahwa penambahan konsentrasi CoCl2 tidak dapat meningkatkan viabilitas dan jumlah agregasi CTC kanker kolorektal.

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Circulating tumor cells (CTCs) are tumor cells that have detached from the primary tumor and circulate in the bloodstream. Culturing CTCs can be beneficial in determining the effective and precise treatments for cancer. However, until now, CTCs culture is still very rare to be successfully done. Cobalt chloride has been reported to enhance tumor cell growth in in-vitro culture, but it has not yet been used to culture colorectal CTCs. Therefore, optimizing the concentration of CoCl2 in culturing colorectal CTCs is essential. Parameters that can be used in this optimization include the cell viability and the aggregates number of CTC. This study aims to investigate the effect of adding different concentrations of CoCl2 (100 and 150 μM) on the aggregates number and cell viability of colorectal CTCs. In this study, isolates obtained from erythrolysis were cultured in a medium with various concentrations of CoCl2 (0, 100, and 150 μM). The cultures were then confirmed with immunofluorescence staining using CK20, PLS3, and DAPI to confirm the presence of colorectal cancer CTCs. Based on the results, all three cultures were confirmed to contain colorectal cancer CTCs. The viability and number of cell aggregates in the culture were observed to be highest at 0 μM, followed by 100 μM, and lowest at 150 μM CoCl2. Based on this study, it can be concluded that the addition of CoCl2 concentrations does not increase the viability and number of aggregates of colorectal cancer CTCs."

"This valuable resource is designed to provide a foundation for understanding major pathophysiological processes, applied pharmacology, and related nursing implications. It includes a holistic framework for assessing major health problems, based on fundamental concepts drawn from biological and behavioral sciences. The book's engaging case study approach builds in complexity with each chapter, illustrating applications of pathophysiology and pharmacology to nursing practice. Content has been assembled by academics and expert clinicians with input from physiologists, pharmacists, medical."