JPH04130248A - Biochemical automatic analyzer - Google Patents
Biochemical automatic analyzerInfo
- Publication number
- JPH04130248A JPH04130248A JP2252304A JP25230490A JPH04130248A JP H04130248 A JPH04130248 A JP H04130248A JP 2252304 A JP2252304 A JP 2252304A JP 25230490 A JP25230490 A JP 25230490A JP H04130248 A JPH04130248 A JP H04130248A
- Authority
- JP
- Japan
- Prior art keywords
- sample
- specimen
- deposited material
- test tube
- abnormal
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
- Granted
Links
- 230000002159 abnormal effect Effects 0.000 claims abstract description 28
- 230000003287 optical effect Effects 0.000 claims abstract description 21
- 238000003756 stirring Methods 0.000 claims abstract description 18
- 102000009123 Fibrin Human genes 0.000 claims abstract description 9
- 108010073385 Fibrin Proteins 0.000 claims abstract description 9
- BWGVNKXGVNDBDI-UHFFFAOYSA-N Fibrin monomer Chemical compound CNC(=O)CNC(=O)CN BWGVNKXGVNDBDI-UHFFFAOYSA-N 0.000 claims abstract description 9
- 229950003499 fibrin Drugs 0.000 claims abstract description 9
- 238000002834 transmittance Methods 0.000 claims abstract description 4
- 239000002244 precipitate Substances 0.000 claims description 35
- 238000004458 analytical method Methods 0.000 claims description 17
- 206010018910 Haemolysis Diseases 0.000 claims description 10
- 230000008588 hemolysis Effects 0.000 claims description 10
- 230000005856 abnormality Effects 0.000 claims description 3
- 238000005070 sampling Methods 0.000 abstract description 21
- 238000005259 measurement Methods 0.000 abstract description 9
- 238000012742 biochemical analysis Methods 0.000 abstract description 6
- 238000004364 calculation method Methods 0.000 description 8
- 239000003153 chemical reaction reagent Substances 0.000 description 8
- 238000010586 diagram Methods 0.000 description 8
- 210000002966 serum Anatomy 0.000 description 6
- 238000000034 method Methods 0.000 description 4
- 230000003595 spectral effect Effects 0.000 description 4
- 238000001514 detection method Methods 0.000 description 3
- 230000000694 effects Effects 0.000 description 3
- 238000000605 extraction Methods 0.000 description 2
- 238000002835 absorbance Methods 0.000 description 1
- 230000005540 biological transmission Effects 0.000 description 1
- 210000004369 blood Anatomy 0.000 description 1
- 239000008280 blood Substances 0.000 description 1
- 238000005516 engineering process Methods 0.000 description 1
- 230000002265 prevention Effects 0.000 description 1
- 238000004611 spectroscopical analysis Methods 0.000 description 1
- 239000000126 substance Substances 0.000 description 1
- 239000002699 waste material Substances 0.000 description 1
Classifications
-
- G—PHYSICS
- G01—MEASURING; TESTING
- G01N—INVESTIGATING OR ANALYSING MATERIALS BY DETERMINING THEIR CHEMICAL OR PHYSICAL PROPERTIES
- G01N35/00—Automatic analysis not limited to methods or materials provided for in any single one of groups G01N1/00 - G01N33/00; Handling materials therefor
- G01N35/00584—Control arrangements for automatic analysers
- G01N35/00594—Quality control, including calibration or testing of components of the analyser
- G01N35/00603—Reinspection of samples
Landscapes
- Engineering & Computer Science (AREA)
- Quality & Reliability (AREA)
- Physics & Mathematics (AREA)
- Health & Medical Sciences (AREA)
- Life Sciences & Earth Sciences (AREA)
- Chemical & Material Sciences (AREA)
- Analytical Chemistry (AREA)
- Biochemistry (AREA)
- General Health & Medical Sciences (AREA)
- General Physics & Mathematics (AREA)
- Immunology (AREA)
- Pathology (AREA)
- Automatic Analysis And Handling Materials Therefor (AREA)
- Investigating Or Analysing Materials By Optical Means (AREA)
- Sampling And Sample Adjustment (AREA)
Abstract
Description
【発明の詳細な説明】
〔産業上の利用分野〕
本発明は生化学自動分析装置に係り、更に詳細には、生
化学自動分析の対象となる検体にフィブリン(糸状もの
)などの析出物を含む異常検体が存在するか否かチェッ
クする機能を備えた生化学自動分析装置に関する。[Detailed Description of the Invention] [Industrial Application Field] The present invention relates to an automatic biochemical analyzer, and more specifically, the present invention relates to an automatic biochemical analyzer, and more specifically, to a biochemical automatic analyzer that contains precipitates such as fibrin (thread-like substances) in a specimen to be subjected to automatic biochemical analysis. The present invention relates to an automatic biochemical analyzer having a function of checking whether or not an abnormal specimen exists.
例えば血清を生化学分析するとき、その検体中に黄色、
溶血、白濁などが生じていると、分析に測定誤差を与え
る要因となる。For example, when performing a biochemical analysis of serum, yellow,
If hemolysis or cloudiness occurs, it will cause measurement errors in analysis.
従来は、このような事態を配慮して、例えば特開昭60
−82865号、特開昭60−187862号公報など
に開示されるように、検体の吸光度を測定する光学的測
定手段を用いて、黄色、溶血、白濁などが生じている異
常検体を事前に検出し、異常検体については、分析対象
から除外する技術が提案されている。Conventionally, in consideration of this situation, for example,
As disclosed in Japanese Patent Application Laid-open No. 82865 and JP-A-60-187862, abnormal specimens with yellow color, hemolysis, cloudiness, etc. are detected in advance by using an optical measuring means that measures the absorbance of the specimen. However, techniques for excluding abnormal samples from analysis targets have been proposed.
前記した異常検体チェック手段は、異常検体に対する無
駄な分析を行わないので、試薬の浪費を防止する利点が
ある。The above-described abnormal sample checking means does not perform unnecessary analysis on abnormal samples, and therefore has the advantage of preventing wastage of reagents.
ところで、異常検体としては、黄色、溶血、白濁のほか
に血清中にフィブリンなどの析出物を含むものが挙げら
れる。この析出物が検体中に存在すると、分析に使用さ
れる光測定の誤差要因になるほかに、検体サンプリング
ノズルの穴づまりの原因になる。従来は、この析出物の
チェックについては充分な配慮がなされていなかった。Incidentally, abnormal specimens include serum that is yellow, hemolyzed, cloudy, and contains precipitates such as fibrin in the serum. If this precipitate exists in the sample, it not only causes errors in optical measurements used in analysis, but also causes clogging of the sample sampling nozzle. Conventionally, sufficient consideration has not been given to checking for this precipitate.
本発明は以上の点に鑑みてなされたもので、その目的と
するところは、生化学分析に際してフィブリンなどの析
出物を含む異常検体を事前にチェックできる機能を備え
た生化学自動分析装置を提供することにある。The present invention has been made in view of the above points, and its purpose is to provide an automatic biochemical analyzer with a function that can check in advance for abnormal specimens containing precipitates such as fibrin during biochemical analysis. It's about doing.
本発明は、上記目的を達成するために、基本的には次の
ような課題解決手段を提案する。In order to achieve the above object, the present invention basically proposes the following problem-solving means.
すなわち、生化学自動分析装置において、フィブリンな
どの析出物を含む異常検体の存在をチェックするために
、試料容器中の検体を撹拌する機構と、前記検体の光の
透過率を測定する光学的測定手段と、前記検体の撹拌に
よる前記光学的測定手段の出力信号の変動分から析出物
に関する情報を求める手段とを備えてなる。In other words, in order to check for the presence of abnormal specimens containing precipitates such as fibrin in automatic biochemical analyzers, there is a mechanism that stirs the specimen in a sample container, and an optical measurement that measures the light transmittance of the specimen. and means for obtaining information regarding precipitates from fluctuations in the output signal of the optical measuring means due to stirring of the sample.
なお、前記光学的測定手段は、試料容器中の検体を分析
する前に検体中の黄色、WJ血、白濁の有無を事前にチ
ェックする光学的測定手段と兼用させることが可能であ
る。Note that the optical measuring means can also be used as an optical measuring means for checking the presence or absence of yellow color, WJ blood, and white turbidity in the specimen before analyzing the specimen in the sample container.
試料容器(例えば試験管)中の検体を撹拌すれば、検体
に析出物が存在している場合には、その析出物が検体中
で移動することになる。When a sample in a sample container (for example, a test tube) is stirred, if a precipitate is present in the sample, the precipitate will move within the sample.
そのため、光学的測定手段に用いる光を検体に透過させ
た時に、移動状態にある析出物がその光透過経路に位置
したり、しなかったりする不定の状態となり、それが光
透過率ひいては光学的測定手段の出力信号の変動となっ
て現われる。Therefore, when the light used for optical measurement means is transmitted through the sample, the moving precipitates may or may not be located in the light transmission path, resulting in an undefined state, which affects the light transmittance and the optical This appears as a fluctuation in the output signal of the measuring means.
従って、この光学的測定手段の出力信号の変動成分がし
きい値を超えるか否か判断するなどして、析出物に関す
る情報が求められる0例えば、光検出信号の変動成分が
規定の値より大きくなった場合には、析出物が存在する
ものと判定し、規定の値より小さい場合には、析出物が
存在しないとの判定を行い、これらの判定を析出物に関
する情報として用いる。なお、析出物の有無だけでなく
、その度合を求めることも可能である。Therefore, information regarding the precipitate is obtained by determining whether the fluctuation component of the output signal of this optical measurement means exceeds a threshold value.For example, if the fluctuation component of the photodetection signal exceeds a specified value. If the value is smaller than a specified value, it is determined that a precipitate does not exist, and these determinations are used as information regarding the precipitate. Note that it is possible to determine not only the presence or absence of precipitates but also their degree.
そして、析出物が存在した時には、その検体を反応容器
側に分注する前に分析対象から除外することで、検体分
注用サンプリングノズルの大づまりを防止することがで
きる。If a precipitate is present, it is possible to prevent the sample dispensing sampling nozzle from becoming clogged by excluding the sample from the analysis target before dispensing the sample into the reaction vessel.
また、析出物が存在する異常検体を取り除くことで、異
常な検体の分析を行うといった無駄をな(すことができ
、しかも光学的分析の信頼性が高まる。Furthermore, by removing abnormal specimens in which precipitates are present, it is possible to eliminate wasteful analysis of abnormal specimens, and moreover, the reliability of optical analysis is increased.
本発明の実施例を図面により説明する。 Embodiments of the present invention will be described with reference to the drawings.
第1図は、本発明の第1実施例を示す要部説明図である
。FIG. 1 is an explanatory diagram of main parts showing a first embodiment of the present invention.
第1図において、1は反応容器、2は検体の入った試験
管、3は試薬容器、4は試験管2から検体を反応容器1
に分注するための検体サンプリング機構、5は試薬容器
3から反応容器lに試薬を分注する試薬分注機構、6は
検体の色情報を得るための光学的測定手段(色センサ)
である0色センサ6は、フォトダイオード、COD (
固体撮像素子)などの受光素子と特定領域の波長の光を
通す光学フィルタより構成される。In Figure 1, 1 is a reaction container, 2 is a test tube containing a sample, 3 is a reagent container, and 4 is a sample from test tube 2 to reaction container 1.
5 is a reagent dispensing mechanism for dispensing the reagent from the reagent container 3 to the reaction container L; 6 is an optical measuring means (color sensor) for obtaining color information of the specimen;
The zero color sensor 6 is a photodiode, COD (
It consists of a light-receiving element (such as a solid-state image sensor) and an optical filter that passes light in a specific wavelength range.
本実施例では、検体の入った多数の試験管2がサンプリ
ングディスク9に格納され、サンプリングディスク9は
間欠的に回転駆動するモータ機構(図示せず)により支
持される。In this embodiment, a large number of test tubes 2 containing specimens are stored in a sampling disk 9, and the sampling disk 9 is supported by a motor mechanism (not shown) that is driven to rotate intermittently.
色センサ6は、サンプリングディスク9の分注位置の前
に配置され、試験管2中の検体の色情報(黄色、溶血、
白濁に関する情報)を、検体を反応容器1側に分注する
前に検知する。The color sensor 6 is placed in front of the dispensing position of the sampling disk 9, and detects color information (yellow, hemolysis, hemolysis, etc.) of the sample in the test tube 2.
Information regarding cloudiness) is detected before dispensing the sample into the reaction vessel 1 side.
検体の黄色、溶血、白濁の分光特性と色センサ6の光学
的フィルタの特性を第3図に示す。第3図のBは青、G
は緑、Rは赤の波長成分を示す。FIG. 3 shows the spectral characteristics of yellow, hemolysis, and cloudiness of the specimen and the characteristics of the optical filter of the color sensor 6. B in Figure 3 is blue, G
indicates the green wavelength component, and R indicates the red wavelength component.
そして、第3図に示すような分光特性をもった検体の色
情報を、色センサ6を用いて測定することにより黄色、
溶血、白濁している検体の色情報を得ることができ、正
常な検体との区別が可能となる。Then, by measuring the color information of the specimen having the spectral characteristics shown in FIG. 3 using the color sensor 6, yellow, yellow,
It is possible to obtain color information on hemolyzed or cloudy specimens, making it possible to distinguish them from normal specimens.
検体の色情報の測定法としては、例えば第2図の(a)
のように検体からの光を色センサ6で単に受光するもの
、同図(b)に示すように試験管2を挾んでランプ11
と色センサ6を備え、検体を通過してきたランプ11の
光を色センサ6で測定する方法、同図(C)に示すよう
に検体中にランプ11と色センサ6を浸して検体の色を
測定する方法などがある。As a method for measuring the color information of a specimen, for example, (a) in Figure 2
The light from the sample is simply received by the color sensor 6, as shown in FIG.
and a color sensor 6, and the color sensor 6 measures the light from the lamp 11 that has passed through the specimen.As shown in FIG. There are various methods of measurement.
7は検体の撹拌機構で、モータにより回転駆動される。Reference numeral 7 denotes a sample stirring mechanism, which is rotationally driven by a motor.
撹拌機構7は、試験管2を着脱可能に支持するホルダ7
aを有し、試験管2をホルダ7aで保持しつつ回転させ
ることで、試験管2中の検体を撹拌する。撹拌機構7は
、試験管2の検体を反応容器1側に分注する位置の手前
に配置される。The stirring mechanism 7 includes a holder 7 that detachably supports the test tube 2.
a, and by rotating the test tube 2 while holding it in the holder 7a, the sample in the test tube 2 is stirred. The stirring mechanism 7 is arranged in front of the position where the sample in the test tube 2 is dispensed into the reaction container 1 side.
ホルダ7aは、サンプリングディスク9が回転する時に
はサンプリングディスク9の試験管2の通過を妨害しな
いように配置され、サンプリングディスク9が一時停止
すると、ホルダ7aが所定(分注位置の手前)の試験管
2をつかむように設定されている。The holder 7a is arranged so as not to obstruct the sampling disk 9 from passing through the test tube 2 when the sampling disk 9 rotates, and when the sampling disk 9 is temporarily stopped, the holder 7a moves the test tube to a predetermined position (before the dispensing position). It is set to grab 2.
8は色センサ6からの出力信号を入力して色信号を演算
する装置である。8 is a device that inputs the output signal from the color sensor 6 and calculates a color signal.
10は主制御装置で、サンプリングディスク9の間欠回
転駆動制御と、検体サンプリング機構4゜試薬分注機構
5の駆動制御と、撹拌機構7の駆動制御とを一連に行い
、かっ色信号演算装置8の情報を得て各試験管2に対す
る検体分注の要否、換言すれば各試験管2中の検体を分
析対象から除外するか否か判定する機能を有する。Reference numeral 10 denotes a main controller, which sequentially controls the intermittent rotation of the sampling disk 9, the specimen sampling mechanism 4, the reagent dispensing mechanism 5, and the stirring mechanism 7, and controls the brown signal calculation device 8. It has a function of determining whether or not a sample is required to be dispensed into each test tube 2 based on the information obtained, in other words, whether or not the sample in each test tube 2 is to be excluded from the analysis target.
次に上記構成よりなる本実施例の動作を説明する。Next, the operation of this embodiment having the above configuration will be explained.
主制御装置10の指令により、サンプリングディスク9
は間欠駆動し、検体分注の手前で血清の色情報及び析出
物の有無をチェックを行う。Based on the command from the main controller 10, the sampling disk 9
is operated intermittently to check the color information of the serum and the presence of precipitates before dispensing the sample.
すなわち、試験管2は、検体分注の手前に来ると撹拌機
構ホルダ7aに支持されて回転撹拌される。この時に、
まず色センサ6により該当試験管2の検体を光学的に分
光測定し、その測定信号が色信号演算装置8に取り込ま
れる。That is, when the test tube 2 comes before sample dispensing, it is supported by the stirring mechanism holder 7a and is rotated and stirred. At this time,
First, the color sensor 6 optically spectrally measures the sample in the test tube 2, and the measurement signal is taken into the color signal calculation device 8.
そして、色センサ6の赤、緑、青の成分の出力をそれぞ
れR,G、Bとすると、血清情報は次式により算出され
る。Then, assuming that the outputs of the red, green, and blue components of the color sensor 6 are R, G, and B, respectively, the serum information is calculated by the following equation.
白濁:L=に−R
黄色: I=l (G−k ’・R)
溶血: H=m (B−l ’ G−にR)ここで、k
、に′、に、2.β′1mは補正係数である。この色情
報り、I、Hの計算と、これらが異常検体のしきい値を
超えたかどうかを色信号演算装置8により行う。White cloudiness: L=to-R Yellow: I=l (G-k'・R) Hemolysis: H=m (B-l' to G-to R) where, k
, ni′, ni, 2. β′1m is a correction coefficient. The color signal calculation device 8 calculates the color information, I, and H, and determines whether or not these exceed the threshold for an abnormal sample.
また、撹拌される検体に析出物が存在する場合には、析
出物が検体中で移動することで、検体における色センサ
の光通過経路に析出物が不定に位置したり、位置しなか
ったりの不定の状態となるので、色センサ6の検出信号
に変動が生じる。In addition, if precipitates are present in the sample being stirred, the precipitates may move within the sample, causing them to be located irregularly or not in the light path of the color sensor in the sample. Since the state is unstable, the detection signal of the color sensor 6 fluctuates.
そして、色信号演算装置8は、この色センサ6の変動が
しきい値を超える時に析出物が存在するものと判定する
。Then, the color signal calculation device 8 determines that a precipitate is present when the fluctuation of the color sensor 6 exceeds a threshold value.
そして、黄色、溶血、白濁、析出物が無いものとの判定
した場合には、その検体は正常なものとして、主制御装
置lOがその検体に対して分注を行うように検体サンプ
リング機構4に指令を与える。If it is determined that the sample is yellow, hemolyzed, cloudy, or free of precipitates, the sample is considered normal, and the main controller IO instructs the sample sampling mechanism 4 to dispense the sample. Give instructions.
一方、黄色、溶血、白濁、析出物のいずれかが存在する
ものと判定された場合には、その検体は異常なものとし
て、主制御装置10がその検体に対しての分注を行わな
いように検体サンプリング機構4に指令を与える。この
ようにして、異常の検体は分析対象から除外される。On the other hand, if it is determined that the sample is yellow, hemolyzed, cloudy, or has precipitates, the main controller 10 determines that the sample is abnormal and prevents the sample from being dispensed. A command is given to the specimen sampling mechanism 4. In this way, abnormal specimens are excluded from the analysis target.
なお、検体の反応容器lへの分注以後の動作(分析動作
)については、既知であるため説明を省略する。Note that the operation (analysis operation) after dispensing the sample into the reaction container 1 is already known, and therefore the description thereof will be omitted.
本実施例によれば、検体に黄色、溶血、白濁がある場合
のほかに、析出物がある場合にもその検体を分析対象か
ら除外するので、異常検体へ投入される試薬の無駄をな
くし試薬の節約を図り得ると共に、分析測定の信頼性を
高めることができる。According to this embodiment, in addition to cases where the sample is yellow, hemolyzed, or cloudy, the sample is also excluded from the analysis when there is precipitate, thereby eliminating waste of reagents that are added to abnormal samples. It is possible to save money and improve the reliability of analytical measurements.
また、検体中に析出物が存在した場合には、その検体の
分注を行わないので、検体サンプリングノズルの穴づま
りを未然に防止することができるといった効果を奏する
。Further, if a precipitate is present in the sample, the sample is not dispensed, so it is possible to prevent the sample sampling nozzle from clogging.
第4図に上記実施例に用いる撹拌機構7の種々のm様を
示す。FIG. 4 shows various types of the stirring mechanism 7 used in the above embodiment.
第4図における(a)は試験管2を水平方向に回転させ
、(b)は試験管2を上下動させ、(C)は試験管2を
横方向に振動させ、(d)は試験管2中に撹拌棒を入れ
ることにより、試験管中の検体を撹拌している。In Fig. 4, (a) rotates the test tube 2 horizontally, (b) moves the test tube 2 up and down, (C) vibrates the test tube 2 laterally, and (d) shows the test tube 2. The sample in the test tube is stirred by inserting a stirring rod into the test tube.
第5図に本発明の第2実施例を示す。FIG. 5 shows a second embodiment of the present invention.
本実施例では、遠心分離装置12と生化学自動分析装置
14を搬送ライン13でつないだシステムを示し、搬送
ライン13の途中に色センサ6及び撹拌機構7を配置、
これらの要素と色信号演算装置8とで血清情報検出装置
を構成する。黄色。This embodiment shows a system in which a centrifugal separator 12 and an automatic biochemical analyzer 14 are connected by a transport line 13, and a color sensor 6 and a stirring mechanism 7 are arranged in the middle of the transport line 13.
These elements and the color signal calculation device 8 constitute a serum information detection device. yellow.
溶血、白濁、析出物の検出は第1実施例同様であるので
、説明を省略する。Detection of hemolysis, cloudiness, and precipitates are the same as in the first embodiment, so their explanations will be omitted.
搬送ライン13には、色センサ6及び撹拌機構7の後段
に異常検体取り出し装置15及び生化学自動分析装置1
4を配置する。The conveyance line 13 includes an abnormal sample extraction device 15 and a biochemical automatic analyzer 1 downstream of the color sensor 6 and the stirring mechanism 7.
Place 4.
本実施例では、搬送ライン13上のサンプルラック17
に格納された試験管2中の検体を順次撹拌しつつ色セン
サ6で分光分析して、黄色、溶血。In this embodiment, the sample rack 17 on the transport line 13
While sequentially stirring the specimen in the test tube 2 stored in the chamber, the color sensor 6 performs spectroscopic analysis to determine that it is yellow and hemolyzed.
白濁、析出物のいずれかの異常の有無を色信号演算部8
が判定する。そして、異常検体があるものと判定される
と、主制御装置10がこの異常検体の試験管2を取り出
すように、異常検体取り出し装置15に指令を与える。The color signal calculation unit 8 determines whether there is any abnormality such as cloudiness or precipitate.
will judge. When it is determined that there is an abnormal sample, the main controller 10 gives a command to the abnormal sample extraction device 15 to remove the test tube 2 containing the abnormal sample.
これにより、該当の試験管2が取り出され、異常検体格
納部16に搬出される。As a result, the test tube 2 in question is taken out and transported to the abnormal sample storage section 16.
なお、異常検体を搬送ライン13上で取り出すのに代え
て、主制御装置10がこの異常検体に対し本来の分析を
行わないという制御指令を生化学分析装置14に送るよ
うにしてもよい。Note that instead of taking out the abnormal sample on the transport line 13, the main controller 10 may send a control command to the biochemical analyzer 14 not to perform the original analysis on this abnormal sample.
第6図に本発明の第3実施例を示す。FIG. 6 shows a third embodiment of the present invention.
本実施例は、搬送ライン13の始端にサンプラ部18を
、後端にサンプル受けを設け、その間に、撹拌機構79
色センサ6、検体サンプリング機構4を配置し、且つ搬
送ライン13の検体サンプリング機構4に隣接させて、
反応容器用のディスク1′及び試薬サンプリング機構5
を配置しである。In this embodiment, a sampler section 18 is provided at the starting end of the conveyance line 13, a sample receiver is provided at the rear end, and a stirring mechanism 79 is provided between them.
The color sensor 6 and the specimen sampling mechanism 4 are arranged, and adjacent to the specimen sampling mechanism 4 of the transport line 13,
Disk 1' for reaction vessel and reagent sampling mechanism 5
It is arranged.
そして1白傷号演算部8が搬送ライン13上にある試験
管2の中から黄色、溶血、白濁、析出物などの異常検体
があるものと判定した場合には、主制御装置10は搬送
ライン13及び検体サンプリング機構4に異常検体を有
する試験管2に対し飛び越し命令を与え、その異常検体
を分析対象から除外する。If the 1 white mark calculation unit 8 determines that there is an abnormal specimen such as yellow, hemolysis, cloudiness, or precipitate in the test tube 2 on the transport line 13, the main controller 10 13 and the sample sampling mechanism 4 are given a skip command to the test tube 2 containing the abnormal sample, and the abnormal sample is excluded from the analysis target.
しかして、第2.第3実施例でも第1実施例と同様の効
果を奏する。However, the second. The third embodiment also provides the same effects as the first embodiment.
以上のように本発明によれば、生化学分析に際してフィ
ブリンなどの析出物を含む異常検体を本来の分析工程の
前に、自動的に事前チェックすることができ、析出物に
よるサンプリングノズルの穴づまり防止や、生化学自動
分析の信頼性を向上させることができる。As described above, according to the present invention, abnormal specimens containing precipitates such as fibrin can be automatically pre-checked before the original analysis process during biochemical analysis, and sampling nozzle holes can be prevented from being clogged with precipitates. prevention and can improve the reliability of automated biochemical analysis.
第1図は本発明の第1実施例を示す要部説明図、第2図
は上記実施例に用いる色センサの具体的態様を示す説明
図、第3図は上記色センサによって黄色、溶血、白濁し
た検体の分光分布特性と光学フィルタの分光特性を示す
説明図、第4図は上記実施例に用いる撹拌機構の具体的
態様を示す説明図、第5図は本発明の第2実施例を示す
説明図、第6図は本発明の第3実施例を示す説明図であ
る。
2・・・検体入り試験管(試料容器)
4・・・検体サンプリング機構、5
6・・・色センサ(光学的測定手段)
8・・・色信号演算装置、9・・・サン10・・・主制
御装置。FIG. 1 is an explanatory diagram of main parts showing a first embodiment of the present invention, FIG. 2 is an explanatory diagram showing a specific aspect of a color sensor used in the above embodiment, and FIG. 3 is an explanatory diagram showing a specific aspect of a color sensor used in the above embodiment. An explanatory diagram showing the spectral distribution characteristics of a cloudy specimen and the spectral characteristics of an optical filter, FIG. 4 is an explanatory diagram showing a specific embodiment of the stirring mechanism used in the above embodiment, and FIG. 5 is an explanatory diagram showing the second embodiment of the present invention. FIG. 6 is an explanatory diagram showing a third embodiment of the present invention. 2... Test tube containing sample (sample container) 4... Sample sampling mechanism, 5 6... Color sensor (optical measurement means) 8... Color signal calculation device, 9... Sun 10...・Main control device.
Claims (1)
出物を含む異常検体の存在をチェックするために、試料
容器中の検体を撹拌する機構と、前記検体の光の透過率
を測定する光学的測定手段と、前記検体の攪拌による前
記光学的測定手段の出力信号の変動分から析出物に関す
る情報を求める手段とを備えてなることを特徴とする生
化学自動分析装置。 2、第1請求項において、前記検体に前記析出物が存在
するか否かのチェックは、前記検体を前記試料容器から
反応容器に分注する前に行うように設定し、前記析出物
が存在するものとの情報が得られると、その検体を分析
対象から除外する手段が設けてある生化学分析装置。 3、試料容器中の検体を分析する前に検体中の黄色、溶
血、白濁に関して事前にチェックする光学的測定手段を
備えた生化学自動分析装置において、前記試料容器中の
検体を攪拌する機構と、この攪拌された検体に前記光学
的測定手段の光を通して得られた光信号の変動成分の解
析より前記検体中にフィブリンなどの析出物が存在する
か否か判定する手段とを設けてなることを特徴とする生
化学自動分析装置。 4、第3請求項において、前記検体に黄色、溶血、白濁
、析出物などの異常が存在するか否かのチェックは、前
記検体を試料容器から反応容器に分注する前に行うよう
に設定し、前記異常の判定がなされると、その検体を分
析対象から除外する手段を備えてなる生化学分析装置。[Claims] 1. In an automatic biochemical analyzer, a mechanism for stirring a specimen in a sample container in order to check the presence of an abnormal specimen containing precipitates such as fibrin, and a light transmittance of the specimen What is claimed is: 1. An automatic biochemical analyzer comprising: an optical measuring means for measuring a sample; and a means for obtaining information regarding precipitates from fluctuations in the output signal of the optical measuring means due to stirring of the specimen. 2. In the first aspect, the presence of the precipitate in the sample is set to be checked before dispensing the sample from the sample container to the reaction container, and the precipitate is present in the sample. A biochemical analyzer is equipped with a means to exclude a sample from analysis if information is obtained that the sample is a sample. 3. In an automatic biochemical analyzer equipped with an optical measuring means for checking yellowness, hemolysis, and cloudiness in a sample before analyzing the sample in the sample container, a mechanism for stirring the sample in the sample container; , means for determining whether or not a precipitate such as fibrin is present in the sample by analyzing a fluctuation component of an optical signal obtained by passing the light of the optical measuring means through the stirred sample. A biochemical automatic analyzer featuring: 4. In the third aspect, checking whether or not there is an abnormality such as yellow color, hemolysis, cloudiness, or precipitate in the specimen is set to be performed before dispensing the specimen from the sample container to the reaction container. The biochemical analyzer further comprises means for excluding the sample from the analysis target when the abnormality is determined.
Priority Applications (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP2252304A JP2825331B2 (en) | 1990-09-21 | 1990-09-21 | Automatic analyzer |
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| JP2252304A JP2825331B2 (en) | 1990-09-21 | 1990-09-21 | Automatic analyzer |
Publications (2)
| Publication Number | Publication Date |
|---|---|
| JPH04130248A true JPH04130248A (en) | 1992-05-01 |
| JP2825331B2 JP2825331B2 (en) | 1998-11-18 |
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ID=17235388
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| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| JP2252304A Expired - Fee Related JP2825331B2 (en) | 1990-09-21 | 1990-09-21 | Automatic analyzer |
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