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  • ¿µ¹®
    ÇѱÛ
  • mean arterial blood pressure
    Æò±Õµ¿¸Æ¾Ð
  • mean blood pressure
    Æò±ÕÇ÷¾Ð
  • occult blood
    ÀáÀçÇ÷¾×, ÀáÇ÷, ¼ûÀºÇ÷¾×
  • occult blood test
    ÀáÇ÷°Ë»ç
  • placental blood
    ŹÝÇ÷¾×
  • pooled blood plasma
    È¥ÇÕÇ÷Àå
  • portal blood pressure
    ¹®¸Æ¾Ð
  • packed red blood cell
    ³óÃàÀûÇ÷±¸
  • percutaneous umbilical blood sampling
    ÇǺΰæÀ¯ÅÈÁÙÇ÷¾×äÃë(¹ý), °æÇÇÁ¦´ëÇ÷¾×äÃë(¹ý)
  • peripheral blood
    ¸»ÃÊÇ÷¾×
  • peripheral blood smear
    ¸»ÃÊÇ÷¾×Æì¹Ù¸¥Ç¥º»
  • red blood cell
    ÀûÇ÷±¸
  • red blood cell dysmorphism
    ÀûÇ÷±¸ÇüÅÂÀÌ»ó(Áõ)
  • red blood corpuscle
    ÀûÇ÷±¸
  • reserve blood
    ¿¹ºñÇ÷·®
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  • ¿µ¹®
    ÇѱÛ
  • differential blood count
    °¨º°Ç÷±¸°è»ê
  • packed red blood cell
    ³óÃàÀûÇ÷±¸
  • red blood cell
    ÀûÇ÷±¸
  • red blood corpuscle
    ÀûÇ÷±¸
  • white blood cell
    ¹éÇ÷±¸
  • white blood corpuscle
    ¹éÇ÷±¸
  • occult blood detection
    ÀáÀçÇ÷¾×°ËÃâ
  • effective blood volume
    À¯È¿Ç÷¾×·®
  • effective renal blood flow
    À¯È¿ÄáÆÏÇ÷·ù·®
  • electromagnetic blood flowmeter
    ÀüÀÚ±âÇ÷·ùÃøÁ¤±â
  • estimated hepatic blood flow
    ÃßÁ¤°£Ç÷·ù·®
  • extrahepatic blood flow
    °£¿ÜÇ÷·ù·®
  • fasting blood sugar
    °øº¹Ç÷´ç, ºó¼ÓÇ÷´ç
  • fat blood level
    Áö¹æÇ÷Ãþ
  • vesical blood fluke
    (¢¡vesical schistosome) ¹æ±¤ÁÖÇ÷ÈíÃæ
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  • ¿µ¹®
    ÇѱÛ
  • blood flow rate
    Ç÷·ù¼Óµµ(úìêüáÜöô).
  • blood flow rate
    Ç÷·ù·®, Ç÷·ù¼Óµµ(úìêüáÜöô).
  • blood flow rate
    Ç÷·ù·®, Ç÷·ù¼Óµµ(úì×µáÜÓø)
  • blood flow velocity
    Ç÷·ù ¼Óµµ (úì×µ áÜÓø)
  • blood flow velocity
    Ç÷·ù¼Óµµ(úì×µáÜÓô).
  • blood flow velocity
    Ç÷·ù¼Óµµ.
  • blood flow volume
    Ç÷·ù·®(úìêüåÖ).
  • blood flowmeter =hemodromometer
    Ç÷·ù°è.
  • blood fluke
    ÁÖÇ÷ÈíÃæ(º´)
  • blood formation
    Ç÷¾×Çü¼º.
  • blood forming organ
    Á¶Ç÷±â°ü(̴̡˻?).
  • blood forming organ
    Á¶Ç÷±â°ü(ðãúìÐïί).
  • blood gas
    Ç÷¾×°¡½º(úìäû- ).
  • blood gas
    Ç÷¾×°¡½º.
  • blood gas
    Ç÷¾×±âü(úìäûѨô÷)
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MN a blood group in the MNSs blood group system; malignant nephrosclerosis; Master of Nursing; meganewt...
MRBC monkey red blood cell; mouse red blood cell
PaO2 partial oxygen tension in arterial blood; partial pressure of oxygen in arterial blood
PBF peripheral blod flow; placental blood flow; pulmonary blood flow
PBL peripheral blood leukocyte; peripheral blood lymphocyte; problem-based learning
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UCP Uncoupling Proteins
ZFP Zinc finger proteins
4E-BPs eIF-4E binding proteins
IGF-BPs high affinity binding proteins
CBF 1--Cerebral blood flow
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  • ¿µ¹®
    ÇѱÛ
    ¼³¸í
  • red blood cell
    ÀûÇ÷±¸
    µ¿ÀǾî=erythrocyte. »ê¼Ò³ª ÀÌ»êȭź¼Ò¸¦ ¿î¹ÝÇÏ´Â Ç÷¾× ³»¿¡ Á¸ÀçÇÏ´Â Ç÷±¸.
  • red blood corpuscle
    ÀûÇ÷±¸
    ¸»ÃÊ Ç÷¾× ¼ººÐÀÇ Çϳª. »ç¶÷¿¡°Ô À־ ¼º¼÷µÈ Á¤»óÀÇ ÇüÀº ÇÙÀÌ ¾ø°í ¾çÂÊÀÌ ¿À¸ñÇÑ ¿øÆÇÀ¸·Î µÇ¾î ÀÖÀ¸¸ç, ±× ÇüÅÂ¿Í Ç÷»ö¼Ò ÇÔ·®¿¡ ÀÇÇÏ¿© »ê¼ÒÀÇ ¼ö¼Û¿¡ ÀûÇÕÇÏ°Ô µÇ¾î ÀÖ´Ù.
  • regenerated blood
    Àç»ý Ç÷¾×
  • renal blood flow
    ½Å Ç÷·ù·®
  • Rh blood group
    Rh Ç÷¾×Çü, ¾Æ¸£ ¿¡ÀÌÄ¡½Ä Ç÷¾×Çü
    1940³â ¹Ì±¹ÀÇ K. ¶õÆ®½´Å¸ÀÌ³Ê µî¿¡ ÀÇÇÏ¿© ¹ß°ßµÈ ÀÓ»óÀûÀ¸·Î ¾ÆÁÖ Áß¿äÇÑ Ç÷¾×Çü. Rh¶ó´Â °ÍÀº, óÀ½¿¡ À̰ÍÀ» °ËÃâÇϴµ¥ ÇÊ¿äÇÑ Ç×Ç÷ûÀ» ¾ò±â À§ÇÏ¿© »ç¿ëÇÑ ¸é¿ª µ¿¹°ÀÎ ºÓÀºÅпø¼þÀÌ
  • S-blood group
    ¿¡½º½Ä Ç÷¾×Çü
    ABO½Ä Ç÷¾×Çü°ú °ü°è ÀÖ´Â Ç÷¾×Çü. Ç÷¾×ÀÇ ºÐºñÇü, ºñºÐºñÇüÀÇ ºÐ·ù¶ó°í Çϸç, 1932³â µ¶ÀÏÀÇ F. ½ÃÇÁ°¡ ¹ß°ßÇÏ¿´´Ù. ABO½Ä Ç÷¾×Çü¿¡ ¼ÓÇÏ´Â Ç׿ø ¹°Áú
  • sensitized red blood cell
    °¨ÀÛ ÀûÇ÷±¸
    °¡¿ë¼ºÀÇ ´Ù´çü ¶Ç´Â ´Ü¹é Ç׿øÀ» °áÇÕ½ÃŲ ÀûÇ÷±¸.
  • sheep blood
    ¾ç Ç÷¾×
  • systemic blood pressure
    üÇ÷¾Ð
  • Ven blood factor
    Ææ Ç÷¾× ÀÎÀÚ
  • venous plasma blood glucose
    Á¤¸Æ Ç÷Àå Ç÷´çÄ¡, Á¤¸Æ Ç÷Àå Ç÷´ç
  • wall of blood vessel
    Ç÷°ü º®
  • white blood cell
    ¹éÇ÷±¸
    ÀûÇ÷±¸¿¡ ºñÇØ Å« ¼¼Æ÷. ¿ÜºÎ·ÎºÎÅÍ Ä§¹üÇÏ´Â ¹ÚÅ׸®¾Æ, ¹ÙÀÌ·¯½º, À̹°ÁúÀ» ޽Ä, Á¦°ÅÇÏ°í ¾Ï¿¡ ÀúÇ×ÇÏ¸ç ¿ì¸® ¸öÀ» ¹æ¾îÇÏ´Â ±â´ÉÀ» °¡Áø´Ù. ÀÎü ³»¿¡ Ç÷¾× 1mm
  • white blood cell count
    ¹éÇ÷¼ö
  • white blood cell transfusion
    ¹éÇ÷±¸ ¼öÇ÷
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oncogene proteins Proteins coded by oncogenes. They include proteins resulting from the fusion of an oncogene and another gene (oncogene proteins, fusion).
(12 Dec 1998)
oncogene proteins, fusion The translation products of the fusion between an oncogene and another gene. The latter may be of viral or cellular origin.
(12 Dec 1998)
oncogene proteins v-abl Transforming proteins encoded by the abl oncogenes. Oncogenic transformation of c-abl to v-abl occurs by insertional activation that results in deletions of specific n-terminal amino acids.
(12 Dec 1998)
oncogene proteins v-erba Transforming proteins encoded by erba oncogenes from the avian erythroblastosis virus. They are truncated versions of c-erba, the thyroid hormone receptor (receptors, thyroid hormone) that have retained both the DNA-binding and hormone-binding domains. Mutations in the hormone-binding domains abolish the transcriptional activation function. V-erba acts as a dominant repressor of c-erba, inducing transformation by disinhibiting proliferation.
(12 Dec 1998)
oncogene proteins v-erbb Transforming proteins encoded by erbb oncogenes from the avian erythroblastosis virus. The protein is a truncated form of the egf receptor (receptors, epidermal growth factor-urogastrone) whose kinase domain is constitutively activated by deletion of the ligand-binding domain.
(12 Dec 1998)
oncogene proteins v-fos Transforming proteins coded by fos oncogenes. These proteins have been found in the finkel-biskis-jinkins (fbj-msv) and finkel-biskis-reilly (fbr-msv) murine sarcoma viruses which induce osteogenic sarcomas in mice. The fbj-msv v-fos gene encodes a p55 kD protein and the fbr-msv v-fos gene encodes a p75 kD fusion protein.
(12 Dec 1998)
oncogene proteins, viral Products of viral oncogenes, most commonly retroviral oncogenes. They usually have transforming and often protein kinase activities.
(12 Dec 1998)
oncogene proteins v-mos Transforming proteins coded by mos oncogenes. The v-mos proteins were originally isolated from the moloney murine sarcoma virus (mo-msv).
(12 Dec 1998)
tau proteins One of the two major classes of microtubule-associated proteins isolated from the brain. The proteins have two domains: one that binds to microtubules and a second that binds to other cell components. By binding to several unpolymerised tubulin molecules simultaneously, tau proteins speed up the nucleation process in tubulin polymerization. Chemically modified tau proteins also appear to be involved in the formation and/or composition of the neurofibrillary tangles and neuropil threads found in alzheimer disease.
(12 Dec 1998)
thyroxine-binding proteins A group of proteins that includes thyroxine-binding globulin, a glycoprotein that serves as the major and specific carrier of thyroxine in plasma, accounting for 70-75% of the bound thyroxine; thyroxine-binding prealbumin, an albumin that serves as the secondary carrier, accounting for between 20 and 25% of the bound thyroxine; and serum albumin, which accounts for the remaining bound thyroxine.
(12 Dec 1998)
egg proteins Proteins which are found in eggs or ova from any species.
(12 Dec 1998)
egg proteins, dietary Proteins found in eggs which are consumed as a food.
(12 Dec 1998)
extracellular matrix proteins Macromolecular organic compounds that contain carbon, hydrogen, oxygen, nitrogen, and usually, sulfur. These macromolecules (proteins) form an intricate meshwork in which cells are embedded to construct tissues. Variations in the relative types of macromolecules and their organization determine the type of extracellular matrix, each adapted to the functional requirements of the tissue. The two main classes of macromolecules that form the extracellular matrix are: glycosaminoglycans, usually linked to proteins (proteoglycans), and fibrous proteins (e.g., collagen, elastin, fibronectins and laminin).
(12 Dec 1998)
extrinsic proteins Pathways that can be easily removed from a biomembrane (e.g., by altering the pH or the ionic strength).
Synonym: extrinsic proteins.
(05 Mar 2000)
UBC proteins <protein> Family of proteins involved in conjugating ubiquitin to proteins.
UBC1, UBC4 and UBC5 have a role in targeting proteins for degradation, but others have more complex roles, including an involvement in cell cycle control (UBC3) and the secretory pathway (UBC6).
(18 Nov 1997)
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