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  • ¿µ¹®
    ÇѱÛ
  • phase wraparound artifact
    À§»óµÑ·¯°ãħÀΰø¹°
  • phase-contrast microscope
    À§»óÂ÷Çö¹Ì°æ
  • plateau phase
    Á¤Á¡Áö¼Ó±â, ÆíÆò±â
  • positive phase
    1. ¾ç¼º»ó 2. Ç×üÁõ°¡±â
  • pachytene phase
    ±½Àº¼¶À¯±â, ÈÄ»ç±â
  • prodromal phase
    Àü±¸±â
  • phase
    1. ±â 2. »ó, À§»ó
  • phase advance
    À§»óÀüÁø
  • phase artifact
    À§»óÀΰø¹°
  • phase axis
    ˤȗ̈
  • phase boundary force
    »ó°èÀü·Â
  • phase boundary potential
    »ó°èÀüÀ§
  • phase coherence
    À§»ó°áÁý
  • phase constant
    À§»ó»ó¼ö
  • phase contrast
    À§»ó´ëÁ¶
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    ÇѱÛ
  • lysogenic phase
    ¿ë¿ø±â
  • manic phase
    Á¶Áõ±â, µé¶ä±â
  • menstrual phase
    ¿ù°æ±â
  • mitosis phase
    À¯»çºÐ¿­±â
  • modulation phase
    º¯Á¶À§»ó
  • phase-contrast microscope
    À§»óÂ÷Çö¹Ì°æ
  • negative phase
    À½¼º±â, À½¼º»ó
  • orgasmic phase
    ±ØÄ¡±â
  • ovogenetic phase
    ³­Àڹ߻ý±â
  • phase
    »ó, ±â, À§»ó
  • pachytene phase
    ±½Àº¼¶À¯±â
  • phase ratio
    »óºñ
  • phase reversal
    À§»ó¹ÝÀü
  • phase rule
    »óÀǹýÄ¢, »ó±ÔÄ¢
  • phase shift
    À§»óº¯À§, À§»óÀ̵¿
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    ÇѱÛ
  • phase encode direction
    À§»ó ºÎȣȭ ¹æÇâ
  • phase encoding
    À§»ó ºÎȣȭ
  • phase encoding gradient
    À§»ó ºÎȣȭ °æ»çµµ
  • phase encoding gradient
    À§»ó ºÎȣȭ °æ»çÀå
  • phase encoding step
    À§»ó ºÎÈ£ ´Ü°è
  • phase evolution of fat suppression
    À§»ó ¼±È¸ Áö¹æ ¾ïÁ¦
  • phase frequency swap
    À§»ó Á֯ļö ±³È¯
  • phase image
    À§»ó ¿µ»ó
  • phase mismapping
    À§»ó ¿ÀÁöµµÀÛ¼º
  • phase of cornification
    °¢Áú±â
  • phase of decline
    °¨Åð±â, °¨¼Ò±â
  • phase of desquamation
    ¹Ú¸®±â
  • phase of incornification
    ºñ°¢Áú±â
  • phase of life problem
    ÀλýÁÖ±âÀÇ ¹®Á¦
  • phase of meditation
    Àẹ±â°£(íÖÜÑÑ¢Êà).
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  • g2 phase
    ÇÕ¼ºÈıâ G2±â
  • gastric phase
    À§»ó(êÖßÓ) À§»êºÐºñ(êÖߤÝÂÝô)ÀÇ .
  • go phase
    Á¤Áö±â Go±â
  • gradient induced phase shift effect
    °æ»ç À¯µµ À§»ó º¯À§ È¿°ú
  • grinding phase
    ºÐ¼â»ó.
  • implantational phase
    Âø»ó±â
  • in-phase image
    À§»ó³» ¿µ»ó
  • inactive phase
    ºñȰµ¿±â
  • inadequate luteal phase
    Ȳü±âºÎÀü(üÜô÷ÐïÝÕîï).
  • inadequate luteal phase
    Ȳü±âºÎÀü(üÜô÷ÐïÝÕîï).
  • inflow phase
    À¯ÀÔ±â(êüìýÑ¢).
  • inspiratory phase
    Èí±â»ó(ýåѨßÓ).
  • inspiratory phase time
    Èí±â»ó½Ã°£.
  • internal phase
    ³»»ó(Ò®ßÓ).
  • intestinal phase
    Àå»ó(íóßÓ) ¡ìÀ§¾×ºÐºñ(êÖäûÝÂÝô)ÀÇ¡í.
KMLE ÀÇÇоà¾î »çÀü À¯»ç °Ë»ö °á°ú : 5 ÆäÀÌÁö: 7
PE Edinburgh Pharmacopoeia; pancreatic extract; paper electrophoresis; partial epilepsy; pelvic examina...
PEAR phase encoded artifact reduction
PLL peripheral light loss; phase-locked loop; poly-L-lysine; pressure length loop; posterior longitudina...
POMP phase-offset multiplanar [pulse sequence in magnetic resonance imaging]; principal outer material pr...
PRC packed red cells; peer review committee; phase response curve; plasma renin concentration; professio...
KMLE ÀÚµ¿ÃßÃâ ÀÇÇоà¾î »çÀü À¯»ç °Ë»ö °á°ú : 5 ÆäÀÌÁö: 7
CA constitutively active
SAM surface active material
SAS surface active substance
APRF 3/acute phase response factor
SPRIA Solid Phase Radioimmune Assay
CancerWEB ¿µ¿µ ÀÇÇлçÀü À¯»ç °Ë»ö °á°ú : 15 ÆäÀÌÁö: 7
phase shift <microscopy> A change in the phase relationship between two alternating quantities of the same frequency.
(05 Aug 1998)
phase variation <microbiology> Alteration in the expression of surface antigens by bacteria.
For example: Salmonella can express either of two forms of flagellin, H1 and H2, that are coded by different genes. Control of which form is expressed is brought about by inversion of the promoter for the H2 gene, which if functional (noninverted) is associated with the expression of H2 and the production of a repressor of the H1 gene.
Inversion occurs about every 1000 bacterial divisions and is under the control of another gene, hin, that is within the invertable sequence.
(31 Dec 1997)
chronic phase Refers to the early stages of chronic myelogenous leukaemia. The number of immature, abnormal white blood cells in the bone marrow and blood is higher than normal, but lower than in the accelerated or blast phase.
(12 Dec 1998)
microscopy, phase-contrast A form of interference microscopy in which variations of the refracting index in the object are converted into variations of intensity in the image. This is achieved by the action of a phase plate.
(12 Dec 1998)
clinical trial, phase I A pre-planned, usually controlled, clinical study of the safety and efficacy of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques based on a small number of healthy persons and conducted over the period of about a year in either the united states or a foreign country.
(12 Dec 1998)
clinical trial, phase II A pre-planned, usually controlled, clinical study of the safety and efficacy of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques based on several hundred volunteers, including a limited number of patients, and conducted over a period of about two years in either the united states or a foreign country.
(12 Dec 1998)
clinical trial, phase III A pre-planned, usually controlled, clinical study of the safety and efficacy of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques after phase II trials. A large enough group of patients is studied and closely monitored by physicians for adverse response to long-term exposure, over a period of about three years in either the united states or a foreign country.
(12 Dec 1998)
clinical trial, phase IV Planned post-marketing studies of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques that have been approved for general sale after clinical trials, phases I, II, and III. These studies, conducted in the united states or a foreign country, often garner additional data about the safety and efficacy of a product.
(12 Dec 1998)
clinical trials, phase I Studies performed to evaluate the safety of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques in healthy subjects and to determine the safe dosage range (if appropriate). These tests also are used to determine pharmacologic and pharmacokinetic properties (toxicity, metabolism, absorption, elimination, and preferred route of administration). They involve a small number of persons and usually last about 1 year. This concept includes phase I studies conducted both in the u.s. And in other countries.
(12 Dec 1998)
clinical trials, phase II Studies that are usually controlled to assess the effectiveness and dosage (if appropriate) of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques. These studies are performed on several hundred volunteers, including a limited number of patients with the target disease or disorder, and last about two years. This concept includes phase II studies conducted in both the u.s. And in other countries.
(12 Dec 1998)
clinical trials, phase III Comparative studies to verify the effectiveness of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques determined in phase II studies. During these trials, patients are monitored closely by physicians to identify any adverse reactions from long-term use. These studies are performed on groups of patients large enough to identify clinically significant responses and usually last about three years. This concept includes phase III studies conducted in both the u.s. And in other countries.
(12 Dec 1998)
clinical trials, phase IV Planned post-marketing studies of diagnostic, therapeutic, or prophylactic drugs, devices, or techniques that have been approved for general sale. These studies are often conducted to obtain additional data about the safety and efficacy of a product. This concept includes phase IV studies conducted in both the u.s. And in other countries.
(12 Dec 1998)
M phase Mitotic phase of cell cycle of eukaryotic cells, as distinct from the remainder, which is known as interphase (and that can be further subdivided as G1, s and G2). Beginning of M is signalled by separation of centrioles, where present and by the condensation of chromatin into chromosomes. M phase ends with the establishment of nuclear membranes around the two daughter nuclei, normally followed immediately by cell division (cytokinesis).
(18 Nov 1997)
M phase promoting factor Protein whose levels rise rapidly just before and fall away just after, mitosis. Thought to be a trigger for mitosis.
(18 Nov 1997)
plateau phase <oncology> Stable stage of disease in multiple myeloma following good response to anti-cancer treatment.
(31 Dec 1997)
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