Mechanism behind autoimmune disorder

Northwestern Medicine scientists discovered a previously-unknown mechanism of disease behind a specific autoimmune disorder. The scientists observed antibodies that targeted phosphatidylethanolamine, an important phosopholipid, from within the endosomes of cells. This discovery was the first observation of a pathogenic mechanism behind anti-phosphatidylethanolamine (aPE) autoimmunity, an immune system disorder that's been correlated with thrombosis, transplant failure and pregnancy loss.

It was first reported decades ago, but exactly how aPE autoimmunity worked had remained a mystery despite a large body of literature documenting its prevalence, according to Ming Zhao, PhD, associate professor of Medicine in the Division of Cardiology and senior author on the paper. Autoimmune diseases usually develop when antibodies-proteins which neutralize pathogens erroneously attack cells while circulating through the bloodstream. To target those cells, the antibodies bind to accessible antigen targets on the exterior surface of cells.

The internalization happens through the endosome, a part of the cell that samples the external environment and gathers in signaling molecules. In this case, the endosome also draws in the antibodies, making the cells vulnerable.This creates an opportunity for anti-PE antibodies that are brought into the cells to bind to the PE in these tiny vesicles and attack the cells from within a miniature 'Trojan Horse' process, this causes chaos within the cell, sending it into an inflammatory state, leading to a greater risk of blood clot formation and pregnancy complications.

It's important to note the inflammatory response may be the principal effect of aPE because it means anti-inflammatory treatment is likely to be more effective than anti-coagulants. These novel discoveries shed light on how cellular vulnerability to aPE is mediated and explain some of its clinical symptoms, according to the study. Because endosomes are an integral part of nearly every type of cell, linking the activity of aPE antibodies to clinical symptoms will be a priority for scientists in future investigations.
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Giapreza for treating low blood pressure

FDA Approves Giapreza (angiotensin II) to treat dangerously low blood pressure. Giapreza (angiotensin II) injection for intravenous infusion to increase blood pressure in adults with septic or other distributive shock. Blood pressure is the force of blood pushing against the walls of the arteries as the heart pumps out blood. Hypotension is abnormally low blood pressure.

 Shock is a critical condition in which blood pressure drops so low that the brain, kidneys and other vital organs can't receive enough blood flow to function properly. In a clinical trial patients with shock and a critically low blood pressure, significantly more patients responded to treatment with Giapreza compared to those treated with placebo.

 Giapreza effectively increased blood pressure when added to conventional treatments used to raise blood pressure. The drug can cause dangerous blood clots with serious consequences (clots in arteries and veins, including deep venous thrombosis); prophylactic treatment for blood clots should be used.
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Mvasi drug for cancer treatment

Mvasi is the first biosimilar approved for the treatment of multiple types of cancer. The is approved for the treatment of adult patients with colorectal, lung, brain, kidney and cervical cancers.

Common side effects of Mvasi include nose bleeds, headache, high blood pressure, inflammation of the nasal cavity, high levels of protein in the urine, taste alteration, dry skin, rectal bleeding, excessive tear production back pain and skin irritation.

Serious side effects of Mvasi include holes in or abnormal connection between two organs, blood clot formation, hypertension, problems in brain function or structure, high levels of protein in the urine and ovarian failure.
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Thrombectomy can prevents stroke complications

Inadequate blood supply to the brain can cause stroke or when blood vessel within the brain ruptures, causing brain tissue to die.

 A stroke is a medical emergency, it requires immediate treatment. During a stroke, the brain does not receive enough oxygen and nutrients, which can leads to death of brain cells.

A thrombectomy is a surgical procedure used to remove a blood clot -thrombus from the brain. The thrombus obstructs blood flow and may cause tissue death.

Thrombectomy is effective in patients with blood clots up to 24 hours after a stroke. Stroke can occur when brain blood vessel bursts.

Thrombectomy is safer than clot-busting drugs because it has no side effects.

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