[ Ana Sayfa | Editörler | Danışma Kurulu | Dergi Hakkında | İçindekiler | Arşiv | Yayın Arama | Yazarlara Bilgi | E-Posta ]
Fırat Üniversitesi Sağlık Bilimleri Tıp Dergisi
2016, Cilt 30, Sayı 1, Sayfa(lar) 031-033
[ Özet ] [ PDF ] [ Benzer Makaleler ] [ Yazara E-Posta ] [ Editöre E-Posta ]
Nadir Bir Tip 1 Diyabet Sunumu; Şiddetli Hiperlipidemi Çocuklar ve Hiperlipideminin Yönetimi: Olgu Sunumu
Sultan KABA, Murat DOĞAN, Keziban BULAN, Yaşar CESUR, Nesrin CEYLAN
Yüzüncü Yıl Üniversitesi, Tıp Fakültesi, Çocuk sağlığı ve Hastalıkları Anabilim Dalı, Van, TÜRKİYE
Anahtar Kelimeler: Diyabetik ketoasidoz, hiperlipidemi, çocuklar
Özet
Diyabetik ketoasidoz, diyabetin en sık, yaşamı tehdit eden, akut bir komplikasyonudur. Lipemik seruma yol açan şiddetli hiperlipidemi, nadiren diyabetik ketoasidoz vakalarında görülür. Burada, ketoasidoz ile başvuran ve sütlü plazma görünümü ve şiddetli hiperlipidemisi olan 10 yaşında bir kız sunulmuştur. Biyokimya çalışmaları için alınmış kan örneğinde süt görünümü vardı. Laboratuvarda, aşırı lipemik numune nedeniyle kan örneği değerlendirilemedi; bu nedenle, yenilenmiş ölçüm yapıldı. İkinci ölçümde, glukoz, trigliserid, toplam kolesterol, düşük yoğunluklu lipoprotein (LDL-kolesterol) ve yüksek yoğunluklu lipoprotein (HDL kolesterol) seviyelerinin yükselmiş olduğu tespit edildi. Diyabetik ketoasidoz, asidotik solunum ve aseton kokusu olan bilinçsiz hastamızda ilk klinik tanı olarak kabul edildi. Bu olgu sunumu ile serum lipit düzeylerinin diyabetik ketoasidozda ve düşük glikoz kontrollü diyabetik çocuklarda ölçülmesi gerektiğini vurguladık. Ayrıca, bu vakada hiperlipidemi yönetimini paylaşmak istedik. Aynı zamanda, kan ölçümlerinin hiperlipidemi koşullarında hatalı olabileceği akılda tutulmalıdır; böylece, hiperlipidemi varlığında laboratuvarı stimüle etmek ikinci bir ölçüm gerektirebilir.
  • Başa Dön
  • Özet
  • Giriş
  • Olgu Sunusu
  • Tartışma
  • Kaynaklar
    • Giriş
    Type 1 diabetes mellitus is the most commonly seen endocrine-metabolism disease of childhood which is characterized by impaired energy homeostasis due to insulin deficiency and diabetic ketoacidosis which is the most commonly seen, life-threatening, acute complication of diabetes mellitus. Over 30% of the patients with newly diagnosed diabetes mellitus manifests by diabetic ketoacidosis. Mild hyperlipidemia in association with diabetic ketoacidosis is a common condition. However, severe hyperlipidemia and milky appearance of plasma is extremely rare1. Particularly in children, there is limited number of cases with an association of severe hyperlipidemia and diabetic ketoacidosis. We presented a case which was diagnosed as type 1 diabetes mellitus and exhibited an association of ketoacidosis and severe hyperlipidemia by laboratory and clinical findings.
  • Başa Dön
  • Özet
  • Giriş
  • Olgu Sunusu
  • Tartışma
  • Kaynaklar
    • Olgu Sunusu
    A 10-years old girl was presented to pediatric emergency department with complaints of vomiting, headache and loss of conscious. She had no fever or diarrhea. Her parents reported that she had polydipsia and polyuria during last 2 days. There was no known risk factor for diabetes mellitus and hyperlipidemia in her personal and family history. In the initial examination loss of conscious, superficial and rapid respiration (kussmaul respiration), severe dehydration and acetone odor were detected; therefore, the patient was admitted to intensive care unit. In the physical examination, following findings were recorded: heart rate, 140 beats/minute; blood pressure 110/70 mmHg; respiration rate 52/minute; body temperature 37°C. Mucosa was dry and capillary filling time was longer than 3 seconds. In auscultation, breath sounds were bilaterally equal, without any abnormal sounds. In abdominal palpation, abdomen was found to be free and no organomegaly was detected. Height was 130 cm (10th percentile) and weight was 24 kg (3-10th percentile). There was no pathological finding in the rest of physical examination. There was a milky appearance in blood sample taken for biochemistry studies. In laboratory, glucose 456 mg/dL, triglyceride (8000 mg/dL; reference range: 0-200 mg/dL), total cholesterol (>1000 mg/dL; reference range: 0-200 mg/dL), low-density lipoprotein (LDL) cholesterol (>800 mg/dL; reference range: 50-159 mg/dL), high-density lipoprotein (HDL) cholesterol (>190 mg/dL; reference range: 35-65 mg/dL), chloride (132 mEq/L; reference range: 98-108 mEq/L), calcium (0,95 mg/dL; reference range: 8.2-10.5 mg/dL), aspartat aminotransferase (AST) (258 U/L reference range: 0-37 U/L), alanine aminotransferase (ALT) (185 U/L; reference range: 0-41 U/) levels were found to be elevated. Complete blood count, coagulation tests and thyroid function tests were normal. BUN, creatinine, total protein, albumin and uric acid levels were also normal. In the urinalysis, the following findings were recorded: color, yellow; density, 1020; glucose, 3+; protein, 2+; hemoglobin, 3+; ketone, 3+. In the blood gas analysis, pH and HCO3 were found as 6.99 and 5 mmol/L, respectively. She had acidemia, ketonuria and clinical findings consistent to diabetic ketoacidosis. In accordance with the management protocol of diabetic ketoacidosis, intravenous fluid and insulin treatment was initiated. Intravenous insulin treatment was replaced by subcutaneous insulin treatment and oral nutrition was permitted on the 24 hour after initiation of intravenous fluid and insulin treatment, when patient became conscious and Ph; >7.30, HCO3; >15 mmol/L, ketone; negative. At the two week of follow-up, triglyceride, total cholesterol and LDL-cholesterol levels gradually returned to normal levels. No treatment was given for hyperlipidemia during this period. Table 1 presents baseline values at admission and final values.


    Büyütmek İçin Tıklayın    		 Table 1: Shows the laboratory values of patient on admission and follow up period

  • Başa Dön
  • Özet
  • Giriş
  • Olgu Sunusu
  • Tartışma
  • Kaynaklar
    • Tartışma
    As diabetic patients with a known diabetes mellitus presents with diabetic ketoacidosis, patients with new onset diabetes mellitus may also manifest with diabetic ketoacidosis. Insulin is involved in protein and lipid metabolism, as well as glucose metabolism. Impaired lipid metabolism in diabetes mellitus has been known for several years2,3. Insulin decreases the use of free fat acids in cytogenesis in liver by inhibiting lipolysis. Also, it enhances degradation of chylomicrons by stimulating lipoprotein lipase. Lipoprotein lipase is an extracellular enzyme which is primarily located at fat tissue and capillary wall of heart and skeletal muscles. Lipoprotein lipase hydrolyzes triglyceride to monoglyceride, fat acid and glycerol. Fat acids are taken by fat tissue and muscles, where they are either used or stored. Chylomicron residues are taken by liver, where they are converted to apolipoprotein, cholesterol esters, cholesterol, fat acids and amino acids. Very low density lipoproteins (VLDLs) synthesized from triglycerides are transported to peripheral tissues and degraded by lipoprotein lipase. Insulin facilitates storage of triglycerides as fat tissue by acting on peripheral lipoprotein lipase4. In case of insulin insufficiency such as uncontrolled diabetes mellitus, mobilization of fat acids is markedly increased, while usage is decreased. This results in increased fat acid load in liver. In patients with insulin insufficiency, enhanced lipolysis and decreased fat acid use and clearance result in hyperlipidemia. As in our case, insulin deficiency causes severe hyperlipidemia in patients with newly onset type 1 diabetes mellitus presented with diabetic ketoacidosis.

    Severe hyperlipidemia has a higher morbidity and mortality when it is complicated by pancreatitis and leads diabetic ketoacidosis5-8. Garnier et al.9 reported that plasma lipid levels were decreased to normal values by insulin therapy in an adult patient with type V hyperlipidemia who presented with diabetic ketoacidosis and pancreatitis. Cole et al.10 reported that hypertriglyceridemia was successfully treated by using low dose unfractionated heparin in an adult patient presented with diabetic ketoacidosis and severe hypertriglyceridemia. Blackett et al.11 reported that they treated a child with diabetic ketoacidosis and hyperlipidemia via insulin treatment alone. In our case, we think the primary illness was diabetes mellitus not primary hyperlipidemia. Therefore we treated the patient with only fluid and insulin treatment. With this treatment the hyperlipidemic and hyperglycemic state were getting to normal gradually. We also did not think pancreatitis due to normal amylase levels.

    Severe lipemia impedes accurate measurements in laboratory test by 3 mechanism: 1) dispersion of light due to turbidity; 2) decrease in sample viscosity and; 3) division between polar and non-polar phases12. Some biochemical parameters are found as high, while some others as low in hyperlipidemia. This is termed as biochemical interference. In a case report by Waseem et al.13, it was found that serum sodium, potassium, chloride and bicarbonate values were low, whereas serum creatinine, triglyceride, total cholesterol were high. In that report, the authors managed their patient by insulin infusion and intravenous fluid therapy according to standard diabetic ketoacidosis protocol. After resolution of diabetic ketoacidosis, hyperlipidemia resolved and serum electrolyte levels returned to normal. In our center, blood glucose measurements are performed by enzymatic hexokinase method. When technical methods were investigated, no information was found about interaction between hyperlipidemia and blood glucose measurements or electrolyte levels. There is information suggesting that lipid levels above 250 mg/dL may lead false-elevation in AST, ALT and creatinine values.

    Abnormally higher triglyceride levels suggest lipoprotein lipase or apolipoprotein C II deficiency. In severe hyperlipidemia caused by insulin deficiency as in diabetes mellitus, a decrease in lipid levels is anticipated when control of diabetes mellitus is achieved or diabetic ketoacidosis is treated. If severe hyperlipidemia persists despite treatment of insulin deficiency, further evaluations are needed for differential diagnosis. In our case, lipid levels returned to normal with insulin therapy and at follow-up hyperlipidemia did not recur in.

    In children, association of severe hyperlipidemia and diabetic ketoacidosis manifested as lipemic serum has been rarely reported. Diabetic ketoacidosis is a condition which is related to high mortality and morbidity. Serum lipid levels must be measured in children with diabetic ketoacidosis or in those with poorly controlled diabetes mellitus. We observed that hyperlipidemia due to diabetes can be controlled successfully with insulin treatment.

    Declaration of Interest
    There is no conflict of interest that could be perceived as prejudicing the impartiality of the research reported.

    Funding
    This research did not receive any specific grant from any funding agency in the public, commercial or not-for-profit sector.
  • Başa Dön
  • Özet
  • Giriş
  • Olgu Sunusu
  • Tartışma
  • Kaynaklar
    • Kaynaklar

    1) Betteridge DJ, Bakowski M, Taylor KG, et al. Treatment of severe diabetic hypertriglyceridaemia by plasma exchange. Lancet 1978; 1: 1368.

    2) Potter JL, Stone RT. Massive hiperlipidemia in diabetic ketoacidosis. The clinicalimportance of laboratory recognition. Clin Pediatr (Phila) 1975; 14: 412-413.

    3) Nyamugunduru G, Roper H. A difficult case. Childhood onset insulin dependent diabetes presenting with severe hyperlipidaemia. BMJ 1997; 314: 62-65.

    4) Farese RV Jr, Yost TJ, Eckel RH. Tissue – spesific regulation of lipoprotein lipase activity by insülin/glucose in normal weight humans. Metabolism 1991; 40: 214-216.

    5) Hsu JH, Wu JR, Chao MC, et al. Severe hyperlipidaemic pancreatitis associated with diabetes. Acta Pediatr 2006; 95: 378-379.

    6) Koul PB, Sussmane JB. Metabolic hyperglycemic emergencies with acute pancreatitis in a child with known insülin – dependent diabetes mellitus. Eur J Emerg Med 2005; 12: 30311.

    7) Shenoy SD, Cody D, Rickett AB, Swift PG. Acute pankreatitis and its association with diabetes mellitus in children. J Pediatr Endocrinol Metab 2004; 17: 1667-1670.

    8) Nair S, Pitchumoni CS. Diabetic ketoasidosis, hyperlipidemia and acute pankreatitis: The enigmatic triangle. Am J Gastroenterol 1997; 92: 1560-1561.

    9) Garnier P, Cailleba A, Lambert M, Moinade S, Maubland C. Association of hyperlipidemia, acute pancreatitis and diabetic keto-acidosiz. A case report (in French). Sem Hop 1980; 56: 2035-2037.

    10) Cole RP. Heparin treatment for severe hypertriglyceridemia in diabetic ketoacidosis. Arch Intern Med 2009; 169: 1439-1441.

    11) Blackett PR, Holcombe HJ, Alaupovic P, Fesmire JD. Plasma lipids and apolipoproteins in a 13-year-old boy with diabetic ketoacidosis and extreme hyperlipidemia. Am J Med Sci 1986; 291: 342-346.

    12) Lutfi R, Huang J, Wong HR. Plasmapheresis to treat hypertriglyceridemia in a child with diabetic ketoacidosis and pancreatitis. Pediatricrics 2012; 129: e195-e198.

    13) Waseem M, Dave-Sharma S, Kin LL, Jara F. Lipemic serum in a toddler with new-onset diabetes mellitus presenting with diabetic ketoasidosis. J Pancreas 2012; 13: 73-75.
  • Başa Dön
  • Özet
  • Giriş
  • Olgu Sunusu
  • Tartışma
  • Kaynaklar
    • [ Başa Dön ] [ Özet ] [ PDF ] [ Benzer Makaleler ] [ Yazara E-Posta ] [ Editöre E-Posta ]
    [ Ana Sayfa | Editörler | Danışma Kurulu | Dergi Hakkında | İçindekiler | Arşiv | Yayın Arama | Yazarlara Bilgi | E-Posta ]