trypanosoma$85538$ - traduzione in olandese
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trypanosoma$85538$ - traduzione in olandese

SPECIES OF KINETOPLASTEA
T brucei; T.brucei; T. brucei; Trypanosoma brucei rhodesiense; Trypanosoma brucei gambiense; Trypanosoma brucei brucei; Trypanosoma gambiense; T. b. gambiense
  • A man having sleeping sickness at Buruma Island, Uganda.
  • Life cycle
  • The six main morphologies of trypanosomatids. The different life cycle stages of ''T brucei'' fall into the trypomastigote and epimastigote morphological categories.

trypanosoma      
n. Trypanosoom (tot de protozoa behorend zweepdiertje dat verschillende soorten ziekten verwekt o.a slaapziekte)

Wikipedia

Trypanosoma brucei

Trypanosoma brucei is a species of parasitic kinetoplastid belonging to the genus Trypanosoma that is present in sub-Saharan Africa. Unlike other protozoan parasites that normally infect blood and tissue cells, it is exclusively extracellular and inhabits the blood plasma and body fluids. It causes deadly vector-borne diseases: African trypanosomiasis or sleeping sickness in humans, and animal trypanosomiasis or nagana in cattle and horses. It is a species complex grouped into three subspecies: T. b. brucei, T. b. gambiense and T. b. rhodesiense. The first is a parasite of non-human mammals and causes nagana, while the latter two are zoonotic infecting both humans and animals and cause African trpanosomiasis.

T. brucei is transmitted between mammal hosts by an insect vector belonging to different species of tsetse fly (Glossina). Transmission occurs by biting during the insect's blood meal. The parasites undergo complex morphological changes as they move between insect and mammal over the course of their life cycle. The mammalian bloodstream forms are notable for their cell surface proteins, variant surface glycoproteins, which undergo remarkable antigenic variation, enabling persistent evasion of host adaptive immunity leading to chronic infection. T. brucei is one of only a few pathogens known to cross the blood brain barrier. There is an urgent need for the development of new drug therapies, as current treatments can have severe side effects and can prove fatal to the patient.

Whilst not historically regarded as T. brucei subspecies due to their different means of transmission, clinical presentation, and loss of kinetoplast DNA, genetic analyses reveal that T. equiperdum and T. evansi are evolved from parasites very similar to T. b. brucei, and are thought to be members of the brucei clade.

The parasite was discovered in 1894 by Sir David Bruce, after whom the scientific name was given in 1899.