cellular level of pathologies

Övningen är skapad 2024-02-29 av feliciajonsssson. Antal frågor: 15.

Klicka

Lär dig orden

Skriv

Stava orden

Lyssna

Lyssna

Spel

Spela spel

Skriv ut

Öva på papper



Välj frågor (15)

Vanligtvis används alla ord som finns i en övning när du förhör dig eller spelar spel. Här kan du välja om du enbart vill öva på ett urval av orden. Denna inställning påverkar både förhöret, spelen, och utskrifterna.

Alla Inga

  • defect in a protein that functions as a chloride ion channel --> ion channel doesnt work cystic fibrosis
  • gain of function and overactivation of the FGFR3 gene --> leads to inhibition of chondrocyte proliferation and differentiation achondroplasia
  • gain of function of FGFR3 gene, ossification is slowed down however this is the least severe variant of its kind hypochondroplasia
  • this pathology has overactivation of the FGFR3 protein which means that this receptor can work even without its ligand (fibroblast growth factors), leads to severe pathology SADDAN
  • FGFR3 overactivation, short limbs, narrow chest and underdevelopment of thorax thanatophoric dysplasia
  • reduced expression of LDL receptor/reduced affinity of receptor and LDL, loss of function familial hypercholesterolemia
  • patient lacks the enzyme protoporphyrinogen oxidase, which means that person cannot turn porphyrin into heme, loss of function variegate porphyria
  • the normal function of HFE is defect, dysregulation of iron metabolism haemochromatosis
  • deficiency of enzyme phenylalanine oxidase --> accumulation of phenylalanine, cannot break down phenylalanine phenylketonuria
  • it is caused by mutations in the LAMP2 gene, leading to impaired autophagy and lysosomal dysfunction, causes accumulation of autophagic vacuoles danon disease
  • deletion of the AZF (azoospermia factor) of the gene azoospermia, oligozoospermia
  • The SHOX protein plays a critical role in regulating chondrocyte differentiation and bone formation, and mutations in the SHOX gene disrupt these processes, resulting in short stature and skeletal abnormalities leri weil syndrome
  • caused by genetic mutations affecting the genes responsible for the production of photopigments (opsin) in cone cells of the retina. daltonism
  • factor VIII 8 is missing (not produced properly or in reduced amount), thus interrupting the cascade and leading to a deficiency in the coagulation activity and a continuous bleeding. haemophilia A
  • factor IX 9 is missing, thus interrupting the cascade and leading to a deficiency in the coagulation activity and a continuous bleeding. Loss of function! haemophilia B

Alla Inga

Utdelad övning

https://glosor.eu/ovning/cellular-level-of-pathologies.11962319.html

Dela