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'''Vyšetřovací metody''' [[Dědičné metabolické poruchy|dědičných metabolických poruch]] jsou sada biochemických, genetických, fyzikálně-vyšetřovacích, anamnestických a jiných postupů k určení konkrétní vrozené enzymatické poruchy, deficitu transportního či jiného proteinu.
'''Screening Methods''' [[Hereditary Metabolic Disorders | Inherited Metabolic Disorders]] are a set of biochemical, genetic, physical-examination, anamnestic, and other procedures to determine a particular congenital enzymatic disorder, deficiency of transport or other protein.  


== Význam diagnózy ==
== Significance of the diagnosis ==
Stanovení diagnózy má vliv zejména na volbu způsobu léčby, která se zásadně liší od chorob spadajících do diferenciální diagnostiky některých dědičných metabolických poruch (onkologická onemocnění, neurodegenerativní onemocnění atd.). Je ale důležité i v případě, kdy pro dané onemocnění neexistuje jiná než symptomatická léčba, kterou je možné provádět i bez znalosti diagnózy. Její význam spočívá mimo upravení léčby také ve zlepšení psychického stavu nemocného po vysvětlení příčin onemocnění a zmírnění úzkosti a nejistoty, dále pak také v umožnění prevence ještě neprojevených příznaků, zbytečných dalších vyšetření a stanovení rizika pro příbuzného probanda.
Diagnosis has an impact mainly on the choice of treatment, which is fundamentally different from diseases falling within the differential diagnosis of some inherited metabolic disorders (oncological diseases, neurodegenerative diseases, etc.). However, it is also important if there is no other than symptomatic treatment for the disease, which can be performed without knowledge of the diagnosis. Its importance lies not only in adjusting the treatment but also in improving the patient's mental state after explaining the causes of the disease and alleviating anxiety and uncertainty, as well as in preventing symptoms that have not yet manifested, unnecessary further examinations and risk assessment for the proband relative.


== Stanovení diagnózy u DMP ==
== Diagnosis of DMP ==


* '''Stanovení diagnózy u konkrétního pacienta'''
* '''Diagnosis of a specific patient'''
{{Podrobnosti|Stanovení diagnózy}}
:Na základě problémů, s kterými pacient přichází, anamnézy a fyzikálního vyšetření jsou indikována vyšetření, která potvrdí či vyvrátí prvotní '''hypotézu'''. V prvním případě je stanovena diagnóza, v druhém případě je vyslovena nová hypotéza a proces se opakuje.
* '''Selektivní screening'''
:U vybrané skupiny lidí, u níž jsou manifestovány některé projevy dědičných metabolických poruch, jsou provedena laboratorní vyšetření některých onemocnění.
* '''Celopopulační screening'''
:Jedná se o aktivní vyhledávání nemocí v celé populaci, umožňuje presymptomatickou diagnostiku.
{{Podrobnosti|Novorozenecký screening}}
:Laboratorní vyšetření na markery onemocnění s velkou incidencí jsou prováděna u všech novorozenců. Musí převažovat benefit (vysoká incidence, závažná onemocnění) nad cenou (finanční náklady, zatížení pacienta a jeho rodiny v případě falešně pozitivního výsledku).


== Úrovně diagnostiky ==
:Based on the patient 's problems, medical history and physical examination, examinations are indicated that confirm or refute the initial''' hypothesis'''. In the first case, a diagnosis is made, in the second case, a new hypothesis is made and the process is repeated.
Dědičnou metabolickou poruchu je možné diagnostikovat u pacienta na několika úrovních, které vyplývají z patogeneze DMP: příčinou je mutace genu, která se projeví enzymovým deficitem; ten způsobí hromadění substrátu a chybění produktu dané metabolické dráhy, což se pak manifestuje jako tkáňové, orgánové či celkové poškození organizmu.
* '''Selective screening'''
: Laboratory examinations of some diseases are performed in a selected group of people in whom some manifestations of inherited metabolic disorders are manifested.
* '''Population-wide screening'''
: It is an active search for diseases in the whole population, it allows presymptomatic diagnosis.


=== Používaná vyšetření ===
: Laboratory tests for markers of diseases with a high incidence are performed in all newborns. The benefit (high incidence, serious illness) must outweigh the price (financial costs, burden on the patient and his family in the event of a false positive result).
Postup: úroveň organismu → úroveň metabolitů → enzymatická úroveň → úroveň nukleových kyselin.
* '''úroveň genetická''' (DNA, mRNA): určení konkrétní mutace metodami DNA diagnostiky – polymerázová řetězová reakce s primery specifickými pro danou mutaci; sekvenace (běžné metody [[sekvenace]], next generation sequencing)
* '''úroveň enzymatická:''' stanovení přítomnosti či lépe aktivity daného enzymu – biochemické stanovení aktivity enzymu: v čase měřen fotometricky, radiometricky, fluorimetricky či hmotnostní spektrometrií úbytek substrátu či kofaktoru nebo vznik produktu stanovované či spřažené reakce. (Pozn. ELISA neměří aktivitu, ale koncentraci enzymu.)
* '''úroveň metabolitů:''' stanovení hromadění substrátu a chybění produktu, někdy i nepřímo (např. hromadění NADH + H<sup>+</sup> u poruch oxidativní fosforylace pomocí stanovení laktátu a 3-hydroxybutyrátu) – biochemicky, imunochemicky, metodami chemické analýzy:
** u '''''malých molekul''''' vysokoúčinná kapalinová chromatografie, plynová chromatografie, u screeningu hojně využívaná tandemová hmotnostní spektrofotometrie
** u '''''komplexních molekul''''' elektroforéza, imunochemie
* '''úroveň organizmu:''' fyzikální vyšetření, anamnéza, zobrazovací metody (např. [[MRI]] u nemocí komplexních molekul kopírujících neurodegenerativní onemocnění příklad!) – nezastupitelné místo. Velkou roli hraje lékař a jeho možnost a schopnost indikovat selektivní screening.


Dostupné laboratorní vyšetření mají různou sensitivitu danou povahou laboratorní metody a analytu.
== Levels of diagnostics ==
An inherited metabolic disorder can be diagnosed in a patient at several levels that result from the pathogenesis of DMP: the cause is a gene mutation that results in an enzyme deficiency; this causes the accumulation of substrate and the absence of the product of the metabolic pathway, which then manifests as tissue, organ or general damage to the organism.


Výstupem je komplexní obraz výsledků, které jsou složité na interpretaci a vyžadují specializaci.
=== Used examinations ===
Procedure: organism level → metabolite level → enzymatic level → nucleic acid level.
* '''genetic level'''(DNA, mRNA): determination of a specific mutation by DNA diagnostic methods - polymerase chain reaction with primers specific for the given mutation; sequencing (common [[sequencing]] methods, next generation sequencing)
* '''enzymatic level:''' determination of the presence or better activity of a given enzyme - biochemical determination of enzyme activity: in time measured photometrically, radiometrically, fluorimetrically or by mass spectrometry loss of substrate or cofactor or formation of product of determined or coupled reaction. (Note: ELISA does not measure activity, but enzyme concentration.)
* '''metabolites level:''' determination of substrate accumulation and product absence, sometimes indirectly (eg NADH + H <sup> + </sup> accumulation in oxidative phosphorylation disorders by determination of lactate and 3-hydroxybutyrate) - biochemically, immunochemically, by chemical analysis methods:
** for '''''small molecules''''', high-performance liquid chromatography, gas chromatography, widely used tandem mass spectrophotometry in screening
** for '''''complex molecules''''' electrophoresis, immunochemistry
* '''organism level:''' physical examination, anamnesis, imaging methods (eg [[MRI]] in diseases of complex molecules replicating neurodegenerative diseases example!) - irreplaceable place. The doctor and his ability and ability to indicate selective screening play a big role.


== Indicie vedoucí k podezření na DMP ==
The available laboratory tests have different sensitivities due to the nature of the laboratory method and analyte.
Důvod k provedení laboratorních vyšetření na genetické, enzymatické úrovni a úrovni metabolitů získá lékař zejména pokud:
* dědičné poruše nasvědčuje '''rodinná anamnéza''' — konsanguinita, podobné projevy u příbuzných, neobjasněná úmrtí v rodině,
* onemocnění považované za běžné '''nereaguje''' na obvyklou léčbu,
* onemocnění je '''multisystémové''',
* onemocnění ovlivňují faktory typické pro DMP — katabolické stavy (horečka, svalová zátěž), hladovění, příjem proteinů nebo sacharidů,
* jsou zjištěny nevysvětlitelné odchylky běžných laboratorních vyšetření,
* manifestované projevy onemocnění jsou vzácné a zároveň typické pro DMP — zápach, barva moči, konkrétní dysmorfie (gargoilizmus) atd.


Projevy se liší u [[Dědičné metabolické poruchy malých molekul#Příznaky|DMP malých molekul]] a [[Dědičné metabolické poruchy komplexních molekul#Příznaky|DMP komplexních molekul]].<br />
The output is a comprehensive picture of results that are difficult to interpret and require specialization.
 
== Indications leading to suspicion of DMP ==
The reason for performing laboratory tests at the genetic, enzymatic and metabolite level is obtained by the doctor especially if:
* hereditary disorders are indicated by a ''family history'' - consanguinity, similar manifestations in relatives, unexplained deaths in the family,
* a disease considered to be '' does not respond '' to normal treatment,
* the disease is '' multisystemic '',
* the disease is affected by factors typical of DMP - catabolic conditions (fever, muscle strain), starvation, protein or carbohydrate intake,
* unexplained deviations from routine laboratory tests are found,
* Manifested manifestations of the disease are rare and at the same time typical for DMP - odor, urine color, specific dysmorphia (gargoilism), etc.
 
Manifestations differ in [[Inherited small molecule metabolic disorders # Symptoms | DMP small molecules]] and [[Inherited complex molecule metabolic disorders # Symptoms | DMP complex molecules]].<br />


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[[Kategorie:Patobiochemie]]
[[Category: Pathobiochemistry]]
[[Kategorie:Pediatrie]]
[[Category: Paediatrics]]
[[Kategorie:Genetika]]
[[Category: Genetics]]
[[File:Screen Shot 2022-04-12 at 8.25.45.png|thumb|782x782px]]


=== Source ===
=== Source ===
* [[ws:Vyšetřovací metody u DMP]]
* [[ws:Vyšetřovací metody u DMP]]

Latest revision as of 23:09, 22 November 2023

Screening Methods Inherited Metabolic Disorders are a set of biochemical, genetic, physical-examination, anamnestic, and other procedures to determine a particular congenital enzymatic disorder, deficiency of transport or other protein.

Significance of the diagnosis[edit | edit source]

Diagnosis has an impact mainly on the choice of treatment, which is fundamentally different from diseases falling within the differential diagnosis of some inherited metabolic disorders (oncological diseases, neurodegenerative diseases, etc.). However, it is also important if there is no other than symptomatic treatment for the disease, which can be performed without knowledge of the diagnosis. Its importance lies not only in adjusting the treatment but also in improving the patient's mental state after explaining the causes of the disease and alleviating anxiety and uncertainty, as well as in preventing symptoms that have not yet manifested, unnecessary further examinations and risk assessment for the proband relative.

Diagnosis of DMP[edit | edit source]

  • Diagnosis of a specific patient
Based on the patient 's problems, medical history and physical examination, examinations are indicated that confirm or refute the initial hypothesis. In the first case, a diagnosis is made, in the second case, a new hypothesis is made and the process is repeated.
  • Selective screening
Laboratory examinations of some diseases are performed in a selected group of people in whom some manifestations of inherited metabolic disorders are manifested.
  • Population-wide screening
It is an active search for diseases in the whole population, it allows presymptomatic diagnosis.
Laboratory tests for markers of diseases with a high incidence are performed in all newborns. The benefit (high incidence, serious illness) must outweigh the price (financial costs, burden on the patient and his family in the event of a false positive result).

Levels of diagnostics[edit | edit source]

An inherited metabolic disorder can be diagnosed in a patient at several levels that result from the pathogenesis of DMP: the cause is a gene mutation that results in an enzyme deficiency; this causes the accumulation of substrate and the absence of the product of the metabolic pathway, which then manifests as tissue, organ or general damage to the organism.

Used examinations[edit | edit source]

Procedure: organism level → metabolite level → enzymatic level → nucleic acid level.

  • genetic level(DNA, mRNA): determination of a specific mutation by DNA diagnostic methods - polymerase chain reaction with primers specific for the given mutation; sequencing (common sequencing methods, next generation sequencing)
  • enzymatic level: determination of the presence or better activity of a given enzyme - biochemical determination of enzyme activity: in time measured photometrically, radiometrically, fluorimetrically or by mass spectrometry loss of substrate or cofactor or formation of product of determined or coupled reaction. (Note: ELISA does not measure activity, but enzyme concentration.)
  • metabolites level: determination of substrate accumulation and product absence, sometimes indirectly (eg NADH + H + accumulation in oxidative phosphorylation disorders by determination of lactate and 3-hydroxybutyrate) - biochemically, immunochemically, by chemical analysis methods:
    • for small molecules, high-performance liquid chromatography, gas chromatography, widely used tandem mass spectrophotometry in screening
    • for complex molecules electrophoresis, immunochemistry
  • organism level: physical examination, anamnesis, imaging methods (eg MRI in diseases of complex molecules replicating neurodegenerative diseases example!) - irreplaceable place. The doctor and his ability and ability to indicate selective screening play a big role.

The available laboratory tests have different sensitivities due to the nature of the laboratory method and analyte.

The output is a comprehensive picture of results that are difficult to interpret and require specialization.

Indications leading to suspicion of DMP[edit | edit source]

The reason for performing laboratory tests at the genetic, enzymatic and metabolite level is obtained by the doctor especially if:

  • hereditary disorders are indicated by a family history - consanguinity, similar manifestations in relatives, unexplained deaths in the family,
  • a disease considered to be does not respond to normal treatment,
  • the disease is multisystemic ,
  • the disease is affected by factors typical of DMP - catabolic conditions (fever, muscle strain), starvation, protein or carbohydrate intake,
  • unexplained deviations from routine laboratory tests are found,
  • Manifested manifestations of the disease are rare and at the same time typical for DMP - odor, urine color, specific dysmorphia (gargoilism), etc.

Manifestations differ in DMP small molecules and DMP complex molecules.

Template:Netisknout

Screen Shot 2022-04-12 at 8.25.45.png

Source[edit | edit source]

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