Vergelijking

Calcitonin (Lachs) vs. Degarelix

Twee peptiden naast elkaar — identiteit, bewijsbasis, juridische status en bekende bijwerkingen.

Identiteit

Categorie

Onderzoek (overig)

CAS-nr.

47931-85-1

214766-78-6

Molecuulmassa

3431.85 g/mol

1632.3 g/mol

Halfwaardetijd

1 h

1320 h

Sequentie

Cys-Ser-Asn-Leu-Ser-Thr-Cys-Val-Leu-Gly-Lys-Leu-Ser-Gln-Glu-Leu-His-Lys-Leu-Gln-Thr-Tyr-Pro-Arg-Thr-Asn-Thr-Gly-Ser-Gly-Thr-Pro-NH2

Ac-D-2Nal-D-4Cpa-D-3Pal-Ser-4Aph(Hor)-D-4Aph(Cbm)-Leu-Ilys-Pro-D-Ala-NH2

Werkingsmechanisme

Calcitonin (Lachs)

Salmon calcitonin binds the calcitonin receptor, which is particularly densely expressed on bone-resorbing osteoclasts. The literature describes that receptor activation inhibits osteoclast activity and motility, thereby reducing bone resorption. This results in reduced release of calcium and phosphate from bone into the blood, which is regarded as the mechanistic basis for the calcium-lowering effect. The salmon variant binds the receptor more strongly and for longer than human calcitonin, which explains its higher potency. Central nervous system mechanisms are additionally discussed in relation to its pain effect in fractures, the basis of which is regarded in the literature as not fully elucidated.

Degarelix

Degarelix is a competitive GnRH receptor antagonist. It binds reversibly and immediately to the pituitary GnRH receptors and blocks their activation. This rapidly suppresses the release of luteinizing hormone (LH) and follicle-stimulating hormone (FSH), which in turn lowers testosterone production in the testes. Unlike GnRH agonists (e.g., leuprorelin), which first cause a transient stimulation with a testosterone surge (flare), this direct antagonism lacks the initial stimulation phase, so testosterone declines without a preceding rise. This mechanism underlies the literature-described use in hormone-dependent prostate cancer.

Bewijsbasis

Hoogste bewijs

Humane RCT

Studies

waarvan bij mensen

Geregistreerde effecten

Openstaande tegenstrijdigheden

Gedocumenteerde bijwerkingen

Juridische status

Country	Calcitonin (Lachs)	Degarelix
Duitsland	Op recept	Op recept
Verenigde Staten	Op recept	Op recept

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Calcitonin (Lachs)

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Degarelix

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Frequently asked questions

What is the difference between Calcitonin (Lachs) and Degarelix?: Calcitonin (Lachs) is classified as "Onderzoek (overig)", while Degarelix is classified as "Onderzoek (overig)". Calcitonin (Lachs): Salmon calcitonin is a synthetically produced 32-amino-acid peptide hormone that corresponds to the body's own calcitonin but exhibits higher biological potency than the human hormone. In the scientific literature it is studied in the context of inhibiting osteoclast-mediated bone resorption and lowering elevated calcium levels. It was historically broadly approved for the treatment of postmenopausal osteoporosis; following European safety reviews, however, its use was restricted. Degarelix: Degarelix (trade name Firmagon) is a synthetic decapeptide and a gonadotropin-releasing hormone (GnRH) receptor antagonist. Unlike GnRH agonists, it blocks the receptor directly and does not trigger an initial testosterone surge (flare). It is an approved prescription medicine for the treatment of advanced, hormone-dependent prostate cancer. This page neutrally summarizes the evidence base and legal status and is not a usage or dosing recommendation. This page contrasts both neutrally and source-based — with no usage or dosing recommendation.
Which peptide is better supported by science, Calcitonin (Lachs) or Degarelix?: The highest available evidence level is "Humane RCT" for Calcitonin (Lachs) and "Humane RCT" for Degarelix. A higher evidence level means more robust data, but says nothing about suitability for an individual. The full body of evidence is on each peptide's own page.
What is the legal status of Calcitonin (Lachs) and Degarelix in Germany and the United States?: Duitsland: Calcitonin (Lachs) — Op recept, Degarelix — Op recept. Verenigde Staten: Calcitonin (Lachs) — Op recept, Degarelix — Op recept. These are factual summaries with source and review date on the individual pages.

Country

Calcitonin (Lachs)

Degarelix

Duitsland

Op recept

Verenigde Staten

Op recept

Frequently asked questions

What is the difference between Calcitonin (Lachs) and Degarelix?

Calcitonin (Lachs) is classified as "Onderzoek (overig)", while Degarelix is classified as "Onderzoek (overig)". Calcitonin (Lachs): Salmon calcitonin is a synthetically produced 32-amino-acid peptide hormone that corresponds to the body's own calcitonin but exhibits higher biological potency than the human hormone. In the scientific literature it is studied in the context of inhibiting osteoclast-mediated bone resorption and lowering elevated calcium levels. It was historically broadly approved for the treatment of postmenopausal osteoporosis; following European safety reviews, however, its use was restricted. Degarelix: Degarelix (trade name Firmagon) is a synthetic decapeptide and a gonadotropin-releasing hormone (GnRH) receptor antagonist. Unlike GnRH agonists, it blocks the receptor directly and does not trigger an initial testosterone surge (flare). It is an approved prescription medicine for the treatment of advanced, hormone-dependent prostate cancer. This page neutrally summarizes the evidence base and legal status and is not a usage or dosing recommendation. This page contrasts both neutrally and source-based — with no usage or dosing recommendation.

Which peptide is better supported by science, Calcitonin (Lachs) or Degarelix?

The highest available evidence level is "Humane RCT" for Calcitonin (Lachs) and "Humane RCT" for Degarelix. A higher evidence level means more robust data, but says nothing about suitability for an individual. The full body of evidence is on each peptide's own page.

What is the legal status of Calcitonin (Lachs) and Degarelix in Germany and the United States?

Duitsland: Calcitonin (Lachs) — Op recept, Degarelix — Op recept. Verenigde Staten: Calcitonin (Lachs) — Op recept, Degarelix — Op recept. These are factual summaries with source and review date on the individual pages.