Isu elisha le-immunotherapy ye-myeloma eminingi

Yabelana ngalokhu okuthunyelwe

Emashumini eminyaka amuva nje, ukwelashwa komdlavuza okusekelwe ku-monoclonal antibody kuye kwasungulwa njengenye yezindlela eziphumelela kakhulu zokwelashwa kwezimila eziqinile kanye nomdlavuza wegazi. Njengoba igama lisho, amasosha omzimba e-monoclonal (mAbs) angamasosha omzimba enziwe ngamaseli ahlanganisiwe asuselwa kumaseli anomzali oyedwa ngakho abelana ngokulandelana okufanayo kwe-amino acid. I-Multiple myeloma iwumdlavuza wegazi ovamile uma kuqhathaniswa, futhi iNyuvesi yase-Osaka eJapane isisungule uhlobo olusha lwe-immunotherapy ukwelapha lesi sifo. 

Ngokwemibiko, kuneziguli ezingaba ngu-18,000 ezine-multiple myeloma eJapan. Yize izinga lokwelashwa lithuthuke kakhulu futhi isikhathi sokuphila kwesiguli sesiluliwe, ukwelashwa okuphelele kunzima kakhulu futhi kuthambekele ekubuyeni.

Ukwelashwa kwe-CAR T-Cell

Molecules sufficient to induce an immune response to produce antibodies-cancer-specific mutations of cell surface proteins are excellent targets. However, mAb therapy against this antigen is impractical because these proteins have great diversity within and between individual tumors, which makes it difficult to identify new cancer-specific target antigens. However, researchers centered on Osaka University in Japan have discovered cancer-specific antigens formed by protein modification, such as glycosylation (the connection of the sugar moiety to the protein) or conformational changes. The research team believes that the new epitope is part of the antigen recognized by immune cells, and can be found by thoroughly searching for cancer-specific mAbs and identifying the antigens it recognizes. figure 2. Overview of Ukwelashwa kwamaseli e-CAR T. Source: Osaka University “We applied this strategy to identify new therapeutic targets for multiple myeloma (MM), Naoki Hosen, the study’s lead author, recently published in Nature Medicine.” Despite progress in MM treatment, relapses continue Is common, so new treatments are needed, including mAb-based treatments. The research team screened more than 10,000 anti-MM mAb clones and identified MMG49 as a mAb that specifically recognizes integrin β7, a cell surface receptor that promotes cell-extracellular matrix adhesion. MMG49 reacts with MM cells , But there are no other bone marrow cell types in the MM patient samples. This prompted the researchers to design a CAR fused with the MMG49 fragment. The MMG49 CAR T produced was found to have an anti-MM effect without destroying normal blood cells. “Our results also show that The active conformation of integrin β7 can be used as an immunotherapy target for MM, ”said study co-author Yukiko Matsunaga. Therefore, even if the expression of the protein itself is not cancer-specific, there are still other cancer immunotherapy targets in many cell surface proteins These targets have not yet been discovered in conformational changes, which is very reasonable. Figure 3. Anti-myeloma activity of MMG49 CAR T cells. Credit: Fred Hutch, Osaka University, researchers provide complex immunotherapy for recurrent immunotherapy, possible Treatment of relapsed leukemia.

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Ukuqonda I-Cytokine Release Syndrome: Izimbangela, Izimpawu, Nokwelashwa
Ukwelashwa kwe-CAR T-Cell

Ukuqonda I-Cytokine Release Syndrome: Izimbangela, Izimpawu, Nokwelashwa

I-Cytokine Release Syndrome (CRS) iwukusabela kwamasosha omzimba okuvame ukubangelwa izindlela zokwelapha ezithile ezifana ne-immunotherapy noma i-CAR-T cell therapy. Kuhilela ukukhululwa ngokweqile kwama-cytokines, okubangela izimpawu ezisukela kumkhuhlane nokukhathala kuya ezinkingeni ezingase zibeke ukuphila engozini njengokulimala kwesitho. Ukuphatha kudinga ukuqapha ngokucophelela kanye namasu okungenelela.

Iqhaza labezimo eziphuthumayo empumelelweni yokwelashwa kwe-CAR T Cell
Ukwelashwa kwe-CAR T-Cell

Iqhaza labezimo eziphuthumayo empumelelweni yokwelashwa kwe-CAR T Cell

Abezimo eziphuthumayo badlala indima ebalulekile empumelelweni yokwelashwa kwe-CAR T-cell ngokuqinisekisa ukunakekelwa kwesiguli okungenamthungo kuyo yonke inqubo yokwelashwa. Banikeza ukwesekwa okubalulekile ngesikhathi sokuthutha, ukuqapha izimpawu ezibalulekile zeziguli, nokuphatha ukungenelela kwezokwelapha eziphuthumayo uma izinkinga ziphakama. Ukusabela kwabo okusheshayo kanye nokunakekelwa kochwepheshe kunomthelela ekuphepheni okuphelele nasekusebenzeni ngempumelelo kokwelashwa, kusiza uguquko olushelelayo phakathi kwezilungiselelo zokunakekelwa kwezempilo kanye nokwenza ngcono imiphumela yesiguli endaweni eyinselele yezindlela zokwelapha ezithuthukisiwe zamaselula.

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