Chromosome 1 : KMLE 의학 검색 엔진 - 의학사전, 의학용어, 의학약어, 의학논문, 약품/의약품 검색

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"Chromosome 1"에 대한 검색 결과입니다. 검색 결과 보는 도중에 Tab 키를 누르시면 검색 창이 선택됩니다.

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Chromosome 2 chromosome 19 chromosome 21 Chromosome 3 chromosome 9 chromosome 8 chromosome 18 Chromosome 17 chromosome 13 chromosome 12

알기쉬운 의학용어풀이집, 서울의대 교수 지제근, 고려의학 출판 유사 검색 결과 : 3 페이지: 1

영문	sex chromosome	한글	성염색체
설명	암수의 성을 결정하는 데 중요한 구실을 하는 염색체. 이것에 대하여 보통의 염색체를 보통염색체라고 한다. 암수의 구별이 있는 생물에서는 암수에 따라 다른 형과 수를 나타내는 염색체이며, 보통염색체에 비해 염색성이나 행동에서 차이가 있다. 특히 동물의 성염색체는 그런 경향이 강하다. 휴지기 및 핵분열 전기에 뚜렷한 이상응축을 나타내며 감수분열 때는 다른 염색체보다 먼저 앞서거나 끌려가는 행동을 보여준다.

영문	chromosome	한글	염색체
설명	유전정보를 담고 있는 DNA가 모여서 이루는 구조물로 핵속에 위치한다. 세포가 분열할 때 이것을 더욱 뚜렷이 관찰할 수가 있다. 이것은 사람처럼 고등생물체에서 너무나 많은 정보를 담고 있어, 엄청난 길이(사람에 있어서 전 DNA를 길이로 따지면 약 2m가 된다)가 된 DNA를 작은 핵이란 공간속에 보관하기 위해서 만들어진 구조이다. 이 염색체의 수는 생물의 종에 따라 다르며 사람의 경우는 46개이다.

영문	chromosome abnormality	한글	염색체이상
설명	염색체의 수나 구조의 이상. 이상이 생긴 세포나 개체는 유전적인 이상을 일으켜 사람의 경우, 다운 증후군-터너 증후군 따위의 여러 가지 형태로 나타난다.

대한의협 의학용어 사전 검색 유사 검색 결과 : 15 페이지: 1

영문

한글
accessory chromosome

덧염색체
acentric chromosome

무중심절염색체
autosomal chromosome

보통염색체, 상염색체
acrocentric chromosome

끝곁매듭염색체
bacterial artificial chromosome

박테리아성인공염색체
bivalent chromosome

이가염색체
circular chromosome

고리염색체
chromosome

염색체
chromosome association

염색체접합
chromosome band

염색체띠
chromosome breakage

염색체손상
chromosome bridge

염색체다리, 염색체교
chromosome chain

염색체사슬, 염색체고리
chromosome configuration

염색체접합형
chromosome grouping

염색체분류(법), 염색체군별(법)

다음

대한의협 필수 의학용어집 사전 검색 유사 검색 결과 : 6 페이지: 1

영문

한글
chromosome

염색체
autosomal chromosome

보통염색체
Philadelphia chromosome

필라델피아염색체
sex chromosome

성염색체
Y chromosome

남성염색체, 와이염색체
chromosome translocation

염색체전위

옛 대한의협 의학용어 사전 검색 유사 검색 결과 : 15 페이지: 1

영문

한글
accessory chromosome

(⇒supernumerary chromosome) 과잉염색체
acentric chromosome

무중심절염색체
acrocentric chromosome

끝곁매듭염색체
autosomal chromosome

보통염색체
chromosome abnormality

염색체이상
chromosome association

염색체접합
bivalent chromosome

두배수염색체
chromosome band

염색체띠
chromosome breakage

염색체손상
chromosome bridge

염색체다리, 염색체교
chromosome

염색체
chromosome chain

염색체사슬, 염색체고리
chromosome configuration

염색체접합형
chromosome grouping

핵형분류
chromosome imbalance

염색체불균형

다음

옛 대한의협 2 의학용어 사전 검색 유사 검색 결과 : 15 페이지: 1

영문

한글
Philadelphia chromosome

필라델피아 염색체
Philadelphia chromosome =Ph

필라델피아 염색체
Philadelpia chromosome

필라델피아염색체
X chromosome

X염색체.
X chromosome

X 염색체
Y chromosome

Y염색체.
accessory chromosome

이성염색체(異性染色體).
acentric chromosome

무중심절염색체(無中心節染色體).
acrocentric chromosome

단부착사형 염색체(端付着絲型染色體), 선단부부착염색체.
acrocentric chromosome

끝곁중심절염색체
anuliform chromosome

고리염색체
arm of chromosome

염색체팔
homologous chromosome

상동염색체(相同染色體).
homologous chromosome

상동염색체
homologous chromosome

상동염색체

다음

옛 대한의협 3 의학용어 사전 검색 유사 검색 결과 : 15 페이지: 1

영문

한글
accessory chromosome

이성염색체(異性染色體).
acentric chromosome

무중심절염색체(無中心節染色體).
acrocentric chromosome

단부착사형 염색체(端付着絲型染色體), 선단부부착염색체.
acrocentric chromosome

끝곁중심절염색체
anuliform chromosome

고리염색체
arm of chromosome

염색체팔
bacterial chromosome

세균염색체
bivalent chromosome

이가염색체(∼染色體).
chromosome

염색체(染色體).
chromosome

염색체
chromosome

염색체재결합.
chromosome

염색체
chromosome

염색체
chromosome

염색체(染色體)
chromosome

염색체

다음

대한해부학회 의학용어 사전 검색 유사 검색 결과 : 15 페이지: 1

영문

한글
Anuliform chromosome

고리염색체
[옛 용어] 윤상염색체
Acrocentric chromosome

끝곁중심절염색체
[옛 용어] 첨동원체염색체
Quadrivalent chromosome

네배수염색체
[옛 용어] 사가염색체
Daughter chromosome

딸염색체
[옛 용어] 낭염색체
Mitochondrial chromosome

사립체염색체
[옛 용어] 사립체염색체
Matrix of chromosome

염색체바탕질
[옛 용어] 염색체기질
Numeral aberration of chromosome

염색체수이상
[옛 용어] 염색체수적이상
Arm of chromosome

염색체팔
[옛 용어] 염색체완
Morphological aberration of chromosome

염색체형태이상
[옛 용어] 염색체형태이상
Satellite chromosome

위성염색체
[옛 용어] 위성염색체
Submetacentric chromosome

중앙곁중심절염색체
[옛 용어] 아중앙동원체염색체
Metacentric chromosome

중앙중심절염색체
[옛 용어] 중앙동원체염색체
Nucleolar chromosome

핵소체염색체
[옛 용어] 핵소체염색체
Nucleolar chromosome

핵소체염색체
[옛 용어] 핵소체염색체,핵인염색체
Univalent chromosome

홑배수염색체
[옛 용어] 단가염색체

다음

대한생화학분자생물학회 용어 사전 검색 유사 검색 결과 : 15 페이지: 1

영문

한글
chromosome

염색체(染色體)
chromosome break

염색체(染色體) 부러짐
chromosome jumping

염색체(染色體) 뛰기
chromosome map

염색체 지도(染色體地圖)
chromosome rearrangement

염색체 재배열(染色體再配烈)
chromosome scaffold

염색체 골격(染色體骨格)
chromosome set

염색체(染色體) 한벌
chromosome substitution

염색체 치환(染色體置換)
chromosome walking

염색체(染色體) 걷기
folded chromosome

접힘 염색체(染色體)
giant chromosome

거대 염색체(巨大染色體)
homoeologous chromosome

부분유사 염색체(部分類似染色體)
homologous chromosome

상동염색체(相同染色體)
lampbrush chromosome

램프솔 염색체(染色體)
limited chromosome

제한염색체(制限染色體)

다음

KI 의학용어 사전 검색 유사 검색 결과 : 1 페이지: 1

영문

한글
chromosome

염색체

KMLE 의학약어 사전 유사 검색 결과 : 5 페이지: 1

Xp	paternal chromosome X; short arm of chromosome X
Xi	inactive X Chromosome
CCA	cephalin cholesterol antigen; chick cell agglutination; chimpanzee coryza agent; choriocarcinoma; ci...
CH	case history; Chediak-Higashi [syndrome]; chiasma; Chinese hamster; chloral hydrate; cholesterol; Ch...
Ch	chest; Chido [antibody]; chief; child; choline; Christchurch [syndrome]; chromosome

다음

KMLE 자동추출 의학약어 사전 유사 검색 결과 : 5 페이지: 1

BAC	Bacterial Artificial Chromosome
CHr	Chromosome
CA	Chromosome aberration
CMGT	Chromosome mediated gene transfer
CCR	Complex chromosome rearrangements

다음

경북대 치과대학 구강내과 교실 사전 유사 검색 결과 : 15 페이지: 1

영문

한글

설명
banding technique chromosome

대상 기술 염색체
chromosome

염색체
chromosome 4

4번 염색체
chromosome aberration

염색체 이상

염색체의 수 및 구조상의 이상. 이상이 생긴 세포 또는 개체는 유전적인 이상을 일으키므로 염색체 돌연변이라고도 한다. 자연적으로 또는 화학적, 물리적인 자극에 의하여 인위적으로도 일어나며 양자 사이에는 양적인 차이는 있어도 질적인 차이는 없다. 변이의 양상은 세포분열 때 또는 침샘 염색체 등에서 관찰된다.【염색체 수의 이상】 정상 체세포는 반수염색체를 가진 정자와 난자의 합체에 의하여 2배체
chromosome abnormality

염색체 이상
chromosome association

염색체 접합
chromosome bridge

염색체 교
chromosome configuration

염색체 접합형
chromosome longarm deletion syndrome

염색체 장지 결손 증후군
chromosome mapping

염색체 지도 작성

특정의 염색체 상에 있는 특정의 유전자 부위를 결정하고, 유전자의 상대적 위치를 나타내는 염색체 지도를 작성하는 과정을 말한다. 기법으로서는 통계적 분석을 이용하는 가계 연구, 체세포 교잡, 염색체 결실 지도의 작성 등을 포함한다.
chromosome monad

일분 염색체
chromosome painting

염색체 페인팅, 염색체 착색
chromosome recombination

염색체 재결합
chromosome-breakage syndrome

염색체-분해 증후군
circular chromosome

환상 염색체

다음

CancerWEB 영영 의학사전 맞춤 검색 결과 : 10 페이지: 1

chromosome 10	10q deletion occurs de novo and shows various malformations, high wide forehead with normocephaly, wide and bulbous tip of the nose, microretrognathia and severe mental retardation. This monosomy is rather rare and is reportedly associated with total colonic aganglionosis with small bowel involvement (TCSA), a variant of Hirschsprung disease. The clinical phenotype of 10p duplication, which is due to malsegregation of a familial translocation, includes severe postnatal growth retardation, profound mental retardation, several major and minor anomalies, dolichocephaly, harelip producing the appearance of a turtle's beak, cleft lip/palate in the absence of harelip, large low set ears, osteoarticular anomalies with hyperflexion of upper limbs and abduction-flexion of lower limbs, etc. Lethality seems considerable. Most cases of trisomy 10qter result from a parental translocation or inversion. More severe clinical manifestations are reported for trisomy 10q24, owing to heart and renal malformations and profound mental retardation. Trisomy 10q25 lacks major malformations, the mental retardation is moderate and the prognosis is favourable. The clinical features include high protruding forehead, round, broad and flat face, fine and arched eyebrows, downward slanting palpebral fissures, blepharophimosis, hypertelorism, hypoplastic and pinched nasal bridge, a small and often beaked nose, cleft palate, ligamentary hyperlaxity, and hypotonia. Inner organ malformations are rare but mental deficiency is severe. 10q monosomy is quite rare and the main features are severe mental retardation, microcephaly, low birth weight, prominent nose bridge, long face, and anomalies of external genitalia. The phenotype of ring chromosome 10 is not very characteristic and includes cardiac and renal anomalies, small stature and moderate mental retardation. Prenatal diagnosis of trisomy 10 is reported. Dysmorphic features include foetal nuchal edema, cleft lip/palate, small lower jaw, rocker-bottom foot, polydactyly, hitch-hiker thumb, syndactyly and inner organ malformations. Genes on chromosome 10 include those encoding glutamate oxaloacetate transaminase, orithine amino transferase and hexokinase 1. Chromosome 10 shows 2 fragile sites in the long arm, 10q23 and 10q25, which probably accounts for its increased involvement in chromosomal anomalies. (05 Mar 2000)
chromosome 11	11p13 monosomy usually occurs de novo and is called the WAGR syndrome. The most constant anomaly is bilateral Aniridia with other ocular anomalies. It is also associated with mental and growth retardation, ambiguous genitalia, nephroblastoma (Wilms tumour) or gonadoblastoma. Familial Aniridia is described with cryptic inversion involving breakpoints within band 11p13. 11p trisomy involving segment 11p12 to 11p14 shows no characteristic ocular anomaly nor signs of malignancy but rather a high convex forehead, frontal upsweep of hair, wide nose bridge, hypertelorism, short wide beaked nose, round chubby cheeks, cleft lip/palate, hypotonia and severe mental retardation. 11p15 duplication shows features of Beckwith-Wiedemann syndrome, macrosomia, dysmorphic facies, cleft palate and mild mental retardation. 11q2 trisomy nearly always results from a malsegregation of a parental translocation. The phenotype includes long prominent philtrum, retracted lower lip, microretrognathia frequently accompanied by malformations of the palate and by glossoptosis, suggestive of Pierre Robin syndrome, preauricular pits and flexion contracture of the limbs. Mental retardation and inner organ malformations are severe. A specific translocation (11;22) involving most frequently breakpoints 11q23 and 22q11 leads to a trisomy with a phenotype very similar to that of 11q2 trisomy. Some additional features probably due to the associated 22 trisomy are preauricular tags, anal atresia or stenosis. The prognosis is characterised by high frequency of early deaths. 11q-syndrome with deletion 11q24 shows congenital heart defects and coarse facial features. The main clinical features of a terminal deletion 11q23 include trigonocephaly, hypertelorism, micrognathia and heart defects. The critical chromosome segment appears to be within the 11q24.1 segment. Considerable growth and mental retardation are usual. The deletion occurs de novo in the majority of cases. Ring chromosome 11 is rare and the phenotype includes mental retardation, failure to thrive/small stature, microcephaly and cafe-au-lait spots. Paracentric inversion inv(11)(q13q25) is associated with polysplenia syndrome including bilateral left sidedness sequence accompanied by complex cardiac malformations and failure of normal asymmetry in morphogenesis. Important genes are localised on chromosome 11, include those for non-alpha globins, whose mutations are responsible for sickle cell anaemia and
chromosome 12	Deletion of the proximal short arm of chromosome 12 is rare and occurs de novo. Microcephaly, narrow forehead, pointed nose and micrognathia are present. Mental and growth retardation are significant but inner organ malformations are generally not present. 12p trisomy nearly always results from a familial translocation. The phenotype includes turricephaly with flat apex, high bulging forehead, flat rectangular face, pronounced hypertelorism, a very short nose with a broad and poorly defined bridge, a short neck with cutaneous folds, ear abnormalities, hypotonia, severe growth and mental retardation and signs of precocious aging in adolescents. Tetrasomy 12p is consistent with Pallister-Killian syndrome. The critical region appears to be confined to 12p11.2. 12q2 trisomy is uncommon and results most frequently from malsegregation of a parental translocation. The patients show a relatively large head with frontal bossing, rectangular face with chubby cheeks and short limbs, especially in the proximal segment. Mental retardation is severe and growth retardation variable. Among others, genes for lactate dehydrogenase B, phenylalanine hydroxylase and haemolytic anaemia due to glyceraldehyde -3-phosphate dehydrogenase deficiency are assigned to chromosome 12. (05 Mar 2000)
chromosome 13	Trisomy 13 or Patau syndrome is characterised by urogenital, cardiac, craniofacial, central nervous system and growth abnormalities. Defects include mental retardation, bilateral harelip and cleft palate, uni- or bilateral hexadactyly, growth retardation, polycystic kidney, ocular abnormalities, congenital heart disease and holoprosencephaly. Over 95% of human trisomy-13 conceptions spontaneously abort. Viable births rarely have prolonged survival. Approximately 80% of the cases involve free 13 trisomy. In 20% of the cases, either a mosaic or trisomy due to a translocation is involved. In cases of mosaicism, the severity of the clinical features can be diminished. A translocation, almost always t(13qDq) and more expressly t(13q14q), can occur de novo or can be transmitted by one of the parents. Rarely, more complex rearrangements are observed. A number of observations of partial 13q trisomies are reported involving segments of variable length, with breakpoints occurring at different sites on 13q. One of the most frequent sites is the interface between q14 and q21. When the trisomy includes the q2 and q3 regions, it leads to a distinctive clinical syndrome. Facial dysmorphism resembles that of Cornelia de Lange syndrome. Respiratory distress and neonatal feeding difficulties are common. A small percentage of partial trisomies is due to de novo duplication. The majority are the result of a malsegregation of a parental rearrangement (a reciprocal translocation or a pericentric inversion). Either total or partial monosomy 13q3 includes rings and terminal deletions and intercalary deletions which include band q14 and are accompanied by a retinoblastoma. The classical "13q-" syndrome is associated with deletions in 13q32. The most distinctive sign is the absence of a defined nasal bridge producing a Greek profile. Microcephaly is often severe with brain malformations. Upper incisors set in a "rabbitlike" forward slant are highly characteristic. Hypoplasia or absence of the thumb, agenesis of the first metacarpal, fusion of the fourth and fifth metacarpals and syndactyly, eye malformations, bone and GI anomalies and considerable growth and mental retardation are frequently found. Deletions limited to bands more proximal to 13q32 are associated with growth retardation and moderate mental retardation, but not with major malformations. Deletions limited to bands distal to 13q32 have severe mental retardation without major malformations and usually without growth failure. The characterization of 13q14 monosomy is justified by the existence of retinoblastoma. From the cytogenetic standpoint, this is a very heterogeneous group, with the deletion capable of extending on both sides of q14, from q11 to q22. The deletion usually occurs de novo and can also result from a parental insertion. In ring 13, certain features of partial or complete 13 trisomy can be seen, due to partial duplication of the rings. The study of patients afflicted with del(13)-retinoblastoma allowed the precise assignment of the gene for esterase D to 13q14.11. Other important genes on chromosome 13 include those for Wilson disease and propionyl CoA-carboxylase. (05 Mar 2000)
chromosome 14	Trisomy 14 occurs de novo and is due to mosaicism. The distinct phenotype includes postnatal growth retardation, psychomotor retardation, prominent forehead, broad nose, dysmorphic ears, cleft or high arched palate, wide mouth, micrognathia, congenital heart disease, a short neck, asymmetry, abnormal skin pigmentation and hypertelorism. Proximal 14 trisomy (14q1 trisomy) is almost always due to a malsegregation from a parental translocation. Growth and mental retardation are severe and the nose is prominent with broad nasal bridge, the upper lip is long with poorly defined philtrum, the mouth resembles the arc of a circle and the Cupid's bow is replaced by a medial notch. The commissures do not form an acute angle but are ovalised by the sagging of the external portions of the lower lip. Hypotelorism is present and anomalies of the limbs are frequent but longevity is generally not impaired. 14q32 trisomy shows macroglossia, mid-face hypoplasia, hypertelorism, umbilical hernia, hepatomegaly, cardiomegaly and moderately delayed psychomotor development. Seizures are reported. Deletion 14(q11.1q13) is associated with hypotelorism, lack of nasal bridge, flattened nasal tip with no visible septum, wide midline cleft of lip and hard palate, ptosis of upper eyelid and semilobar holoprosencephaly. Ring chromosome 14 shows seizures, mild facial dysmorphism, developmental and moderate growth delay. Chromosome 14 carries the family of genes which encode the heavy chain of immunoglobulins. (05 Mar 2000)
chromosome 15	Mosaic trisomy 15 is reported with no major or visible dysmorphia and severe inner organ defect. Duplication in the 15q11-13 region is also reported, although rarely, and can be associated with Prader-Willi syndrome. The phenotype includes developmental delay, particularly concerning acquisition of speech, ataxic gait with similarities to Angelman syndrome and seizures. Craniofacial dysmorphism includes oval face, high cheekbones and deep orbits. The trisomy can result from a malsegregation of a parental translocation, or can occur de novo with the presence of a supernumerary acrocentric chromosome of the size of a G-group chromosome or a supernumerary chromosome carrying satellites at both extremities. The latter rearrangement causes partial 15 tetrasomy results from an inverted duplication of chromosome 15. Patients with inv dup(15) show normal growth, moderate to severe mental retardation, seizures, poor motor coordination, behavioural problems, autism and mild dysmorphic features. Triplication in the same 15q11-13 region is also reported. Clinically, the patients present with hypotonia, developmental delay, visual impairment and minor dysmorphic features. 15q2 trisomy results from malsegregation of a parental translocation and shows a highly characteristic craniofacial dysmorphism including microdolichocephaly, narrow palpebral fissures, protuberant philtral borders and micrognathia. Various osteoarticular anomalies are observed. Inner organ malformations include heart disease. Mental retardation is severe. Prader-Willi syndrome and Angelman syndrome are distinct mental retardation disorders which result from paternal and maternal deficiency, respectively, for chromosome 15q11-q13. Approximately half of the patients with Prader-Willi syndrome show microscopically detectable paternally derived deletions, duplications and other chromosomal rearrangements of 15q11.2, or maternal uniparental disomy for chromosome 15. In contrast, Angelman syndrome can result from either maternally inherited deletions of this region or paternal uniparental disomy for chromosome 15. Major features of Prader-Willi syndrome include neonatal hypotonia with feeding difficulties, poor spontaneous movement, spells of cyanosis, a weak or absent cry, hypogonadism with cryptorchidism, mental retardation, obesity, hyperphagia and short stature. Features of Angelman syndrome include severe mental deficiency, ataxic (puppet-like) gait, prognathia and wide mouth, seizures and paroxysmal laughter. The phenotype of an interstitial deletion 15q13 includes gross congenital anomalies consisting of large fontanelles and sutures, midface hypoplasia, flat ears with thin cartilage, prominent eyes, anteverted nostrils, cleft palate, positional deformation of hands and feet, hypertonia and inner organ malformations. The phenotype shows few overlapping features with Prader-Willi syndrome or Angelman syndrome. Ring chromosome 15 is a rare cytogenetic disorder characterised by growth retardation, microcephaly, triangular facies, hypertelorism, brachydactyly, variable mental retardation and speech delay. Gene assignments to chromosome 15 include the gene coding for hexosaminidase-A, whose mutation causes Tay-Sachs disease, and the major gene for Marfan syndrome. (05 Mar 2000)
chromosome 16	Trisomy 16, the most common autosomal aneuploidy encountered in spontaneous abortuses, is rarely diagnosed in ongoing pregnancies and is considered lethal. However, cases of trisomy 16 mosaicism ascertained either by amniocentesis or in liveborn infants are reported. The liveborns exhibit a distinct and recognizable phenotype of highly variable severity, with multiple congenital anomalies and dysmorphic features including asymmetry, intrauterine growth retardation, congenital heart disease, respiratory tract and musculoskeletal defects. The phenotype of 16p trisomy includes considerable intrauterine and postnatal growth retardation, small round skull, scant lashes and eyebrows, round flat face, prominent maxillae, micrognathia, round low-set ears with hypoplastic tragus and helix and protuberant anthelix, aplasia or hypoplasia of the thumb and severe mental impairment. All reported cases of complete or partial duplication of 16q result from a parental translocation. Frequent findings include growth retardation, mental handicap, asymmetrical head, high forehead, short prominent or beaked nose, long philtrum and thin upper lip. Osteoarticular and perineal anomalies are constant. Duplication 16q13 shows multiple malformations including ambiguous genitalia, congenital heart disease, syndactyly and unusual facies including downslanting palpebral fissures, low set ears with severe unilateral microtia, micrognathia and cleft palate. Chromosome 16 gene assignments include the alpha-globin genes, whose mutations cause thalassaemias, and the genes for haptoglobin, adult polycystic kidney disease, and others. (05 Mar 2000)
Chromosome 17	Chromosome 17 imbalances are not compatible with life. The phenotype of 17q2 trisomy, which is caused by a malsegregation of a parental translocation, includes microcephaly with high forehead, frontal bossing, high hairline with widow's peak, short thick neck, squinty eyes, large mouth with downturned corners, brachyrhizomelia, hexadactyly and severe mental retardation. Severe inner organ malformations are reported in patients with trisomy 17q23. Charcot-Marie-Tooth is the most common peripheral neuropathy, occurring at a frequency of 1 in 2500. The most prevalent form of the disease, type 1 Charcot-Marie-Tooth , is characterised by significantly reduced nerve conduction velocities. The disease phenotype has been shown to segregate with a submicroscopic DNA duplication within 17p11.2, and Charcot-Marie-Tooth 1a patients are reported with cytogenetically visible duplication of 17p11.1-17p12. The disease phenotype is probably due to a gene dosage effect. Miller-Dieker syndrome is comprised of a characteristic facial appearance and lissencephaly (smooth brain). Most Miller-Dieker syndrome patients have microdeletions of 17p13.3, detectable cytogenetically or submicroscopically. Smith-Magenis syndrome is a clinically recognizable multiple congenital anomaly/MR syndrome associated with deletion of chromosome 17(p11.2). The patients show dysmorphic features including broad flat midface with brachycephaly, broad nasal bridge, brachydactyly, speech delay and hoarse deep voice, short stature, developmental delay and self- destructive behaviour, primarily onychotillomania and polyembolokoilamania, and sleep disturbances. Gene assignments include the p53 tumour suppressor, Charcot-Marie-Tooth type 1a,8 galactokinase and Niemann-Pick disease. (05 Mar 2000)
chromosome 18	Edwards syndrome (trisomy 18), the second most common autosomal trisomy with an occurrence rate of 1 in 8,000 live births, is associated with a distinct pattern of dysmorphogenesis and congenital abnormalities which results in early death. Marked growth deficiency is a major trait of the phenotype. Other striking clinical features of this syndrome include congenital heart abnormalities, mental and developmental delays, prominent occiput, faunlike ears, micrognathia, short sternum, narrow pelvis, overlapping fingers and rocker-bottom feet. The 18q12.2 subband is identified as the critical region in the trisomy 18 phenotype. Trisomy 18 mosaicism can present with minimal non-specific signs and no typical stigmata of the full trisomy. Although Edwards syndrome is typically associated with duplication of the entire chromosome 18, several individuals with partial trisomies of chromosome 18 (18q2 trisomy, 18p & q1 trisomy) are reported. These patients display a range of severity from a relatively mild phenotype with no internal organ malformations to the classic characteristics of Edwards syndrome. Isochromosome 18p [i(18p)] is described 6 and is associated with a distinctive syndrome, tetrasomy 18p, which includes low birth weight, characteristic facies, neonatal hypotonia with subsequent limb spasticity, short stature, microcephaly, mental retardation and seizure disorders. Isochromosome 18q is a rare cytogenetic abnormality resulting in trisomy for the q arm and monosomy for the p arm of chromosome 18. Phenotypic characteristics are not yet fully delineated. Clinical and pathological examination reveals features characteristic of both trisomy 18 and monosomy 18p or features characteristic of trisomy 18 alone. Severe cephalic malformations such as holoprosencephaly, cebocephaly and cyclopia are reported in i(18q), but are rarely described in trisomy 18 and are only occasional findings in monosomy 18p. Isodicentric chromosome 18 was described and the clinical findings are associated with both the trisomy 18 and 18p- syndromes. The 18q- syndrome or 18q2 monosomy is a well-described partial aneusomy disorder resulting from the deletion of a portion of the long arm of chromosome 18. Typically, patients with this syndrome show growth deficiency, dysmorphic facial features, limb defects, genitourinary malformations, neurologic and ocular anomalies, and developmental delay with mental retardation. The dysmorphic features are mild and include midfacial hypoplasia, carp-shaped mouth and abnormally folded ears. Neurologic findings consist of hypotonia, poor coordination, choreoathetotic movements and ophthalmologic abnormalities. Proximal interstitial deletion of 18q involving band 18q12.3 is recognised with a distinctive phenotype including moderate to severe MR, high forehead, deep-set eyes, hypotelorism, flat nasal bridge, dysplastic ears, excess dermatoglyphic whorls and aggressive behaviour. In the majority of deletions of the short arm of chromosome 18 (18p monosomy or 18p- syndrome), dysmorphism is not very distinctive. Psychomotor retardation is more or less severe. The ring 18 phenotype shares features of the 18p- syndrome and those of the 18q- syndrome with predominance of the features of the 18q monosomy. Mosaicism is frequently observed with ring chromosomes. The gene for peptidase A is localised to 18q23. (05 Mar 2000)
chromosome 19	The phenotype of 19q trisomy, which is caused by malsegregation from familial translocation, includes microcephaly with brachycephaly, flat face, widely gaping cranial sutures, hypertelorism and palpebral ptosis, fishlike mouth, short neck, small pudgy hands and feet, growth retardation, slight to very severe mental retardation. Duplication of 19p13.1 and part of 19p13.2 is associated with developmental delay, unusual lower facial features including vertical ridging on the chin, extra philtral pillar, midline ridge on the anterior portion of the tongue and congenital heart defect. A placental karyotype of nonmosaic trisomy 19 was described with an abnormal foetus surviving to midtrimester. Gene assignments on chromosome 19 include the gene for myotonic dystrophy at 19q13.3, Lewis and Lutheran blood groups and the chorionic gonadotrophin

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accessory chromosome	A chromosome existing without its normal homologous chromosome; at the reduction division of gametogenesis an accessory chromosome is likely to be included in one daughter cell and not in the other, but may be lost completely by lagging behind on the equatorial plate. Synonym: monosome, odd chromosome, unpaired allosome, unpaired chromosome. (05 Mar 2000)
acentric chromosome	A fragment of a chromosome lacking a centromere and unable to attach to the mitotic spindle, therefore unable to take part in the division of a nucleus and randomly distributed in daughter cells. Synonym: acentric fragment. (05 Mar 2000)
acrocentric chromosome	A chromosome with the centromere placed very close to one end so that the short arm is very small, often with a satellite. (05 Mar 2000)
balanced chromosome	<genetics> A chromosome which is unable to pair with its homologue and participate in homologus recombination during meiosis because it contains several inversion mutations (that is, has segments which have become flip-flopped). (09 Oct 1997)
B chromosome	<genetics> Small acentric chromosome, part of the normal genome of some races and species of plants. (18 Nov 1997)
bivalent chromosome	A pair of chromosome's temporarily united. (05 Mar 2000)
male chromosome complement	The large majority of males have a 46, xy chromosome complement (46 chromosomes including an x and a y chromosome). A minority of males have other chromosome constitutions such as 47,xxy (47 chromosomes including two x chromosomes and a y chromosome) and 47,xyy (47 chromosomes including an x and two y chromosomes). (12 Dec 1998)
marker chromosome	An abnormal chromosome that is distinctive in appearance but not fully identified. For example, the fragile x chromosome was once called the marker x. (12 Dec 1998)
p arm of a chromosome	The short arm of a chromosome (from the french petit meaning small). All human chromosomes have 2 arms: the p and q arms. (12 Dec 1998)
giant chromosome	<cell biology> Giant chromosomes produced by the successive replication of homologous pairs of chromosomes, joined together (synapsed) without chromosome separation or nuclear division. They thus consist of many up to 1000) identical chromosomes (strictly chromatids) running parallel and in strict register. The chromosomes remain visible during interphase and are found in some ciliates, ovule cells in angiosperms and in larval Dipteran tissue. The best known polytene chromosomes are those of the salivary gland of the larvae of Drosophila melanogaster which appear as a series of dense bands interspersed by light interbands, in a pattern characteristic for each chromosome. The bands, of which there are about 5,000 in Drosophila melanogaster, contain most of the DNA (ca 95%) of the chromosomes and each band roughly represents one gene. The banding pattern of polytene chromosomes provides a visible map to compare with the linkage map determined by genetic studies. Some segments of polytene chromosome show chromosome puffs, areas of high transcription. (18 Nov 1997)
Giemsa chromosome banding stain	<technique> A unique chromosome staining technique, used in human cytogenetics to identify individual chromosomes, which produces characteristic bands. It utilises acetic acid fixation, air drying, denaturing chromosomes mildly with proteolytic enzymes, salts, heat, detergents, or urea, and finally Giemsa stain; chromosome bands appear similar to those fluorochromed by Q-banding stain. Synonym: Giemsa chromosome banding stain. (05 Mar 2000)
metacentric chromosome	A chromosome with a centrally placed centromere that divides the chromosome into two arms of approximately equal length. (05 Mar 2000)
ring chromosome	A structurally abnormal chromosome in which the end of each chromosome arm has been lost and the broken arms have been reunited in ring formation. A ring chromosome is denoted by the symbol r. (12 Dec 1998)
Christchurch chromosome	An abnormal small acrocentric chromosome (no. 21 or 22) with complete or almost complete deletion of the short arm; found in cultured leukocytes in some cases of chronic lymphocytic leukaemia, also in some normal relatives of patients. (05 Mar 2000)
chromosome	<cell biology> The self-replicating genetic structures of cells containing the cellular DNA that bears in its nucleotide sequence the linear array of genes. The DNA of eukaryotes is subdivided into chromosomes, that consist of a number of chromosomes whose DNA is associated with various proteins. The chromosomes become more tightly packed at mitosis and become aligned on the metaphase plate. Each chromosome has a characteristic length and banding pattern. In prokaryotes, chromosomal DNA is circular, and the entire genome is carried on one chromosome. See: C banding, G banding. (10 Nov 1998)

다음

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A chromosome

A염색체(과잉 염색체 이외의 보통 염색체)
Philadephia chromosome

필라델피아 염색체
X chromosome

X염색체
Y chromosome

Y염색체
chromosome

염색체
chromosome number

염색체수
chromosome translocation

염색체 전좌
criminal chromosome

범죄자 염색체(남성의 극히 일부에 보이는 여분의 Y염색체)
sex chromosome

성염색체
x-chromosome

염색체

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