Orian Darvenn

🚨😱 LA TECHNOLOGIE QUI VA CHANGER LA VIE DES PERSONNES ÂGÉES Regardez ces grands-parents avec un exosquelette Haier (made in China) : Ils marchent à nouveau normalement, avec fluidité, comme s’ils avaient 20 ans de moins ! 🔥👴👵 La liberté de mouvement retrouvée… c’est impressionnant.

🗣 Professor Dr. Klinghardt sagt Unglaubliches: Der größte Vergiftungsfaktor auf dem Planeten Erde sind nicht Pestizide. Nicht das Deo. Nicht Plastikflaschen. Nicht Aluminiumkochtöpfe. Es sind Chemtrails. 🛩 Aluminium... 🛩 Barium... 🛩 Strontium... 🛩 Schwermetalle... Tonnen davon prasseln auf uns nieder – Tag für Tag, Jahr für Jahr. Das Schlimmste: Das Aluminiumgehalt in unserem Nervensystem ist in den letzten Jahren exponentiell angestiegen. Klinghardt sagt klar: Die Folgen sind Autismus, Lernstörungen bei Kindern, MS, ALS, Parkinson, Neuropathien & chronische Erkrankungen. Die einzige Frage, die jetzt zählt: Wie bekommen wir dieses Gift wieder raus aus dem Körper? 🏔 Es gibt eine natürliche Substanz, die genau das kann – & sie entgiftet anders als jedes andere Mittel auf der Welt: SHILAJIT. ● Was Shilajit so anders macht: Der Hauptbestandteil sind Humin- & Fulvinsäuren – organische Säuren, die Toxine binden. So weit nichts Neues. ● Doch jetzt kommt der entscheidende Punkt: Shilajit enthält diese Säuren im kompletten Größenspektrum von 1:150. Die längste Huminsäurekette ist 150-mal länger als die kürzeste. ● Warum das alles verändert: Die Größe des Moleküls bestimmt, welches Toxin gebunden wird. Klein bindet klein. Groß bindet groß. 🪨 Zeolith → bindet Ammoniak, ein paar bestimmte Toxine 🌿 Chlorella → bindet Quecksilber, einige Schwermetalle ⬛️ Aktivkohle → bindet größere organische Moleküle 🏔 Shilajit → bindet ALLES. Von winzigsten bakteriellen Giftstoffen bis zu großen Aluminium- & Schwermetallverbindungen. Genau das, was laut Klinghardt aus der Luft auf uns niederprasselt & ohne Rückvergiftung. Was einmal gebunden ist, bleibt gebunden & verlässt den Körper. Ohne Kopfschmerzen. Ohne Entgiftungskrise. Jeder kennt sie doch

✨TON CORPS N'EST PAS FAIT D'EAU, IL EST FAIT DE CRISTAUX LIQUIDES, ET ILS ONT BROYÉ LE SIGNAL ! On t'a appris que le corps humain est composé à 70% d'eau.. Imagine un ballon biologique rempli de la même substance qui sort de ton robinet. C'est la plus grande simplification excessive de la biologie moderne. L'eau à l'intérieur de tes cellules, ce n'est pas de l'eau normale, c'est de l'Eau Structurée — une quatrième phase de l'eau découverte par le Dr. Gerald Pollack de l'Université de Washington.. pas solide.. Pas liquide, pas gazeuse. Une phase gélatineuse et cristalline, qui conduit l'électricité, stocke des informations, et communique par fréquence électromagnétique. Le Dr. Pollack a démontré, que lorsque l'eau est exposée à la lumière infrarouge, elle forme spontanément une "Zone d'Exclusion" — une couche de molécules parfaitement organisées qui génère une charge électrique. Tes cellules sont recouvertes de cette eau.. C'est la batterie qui alimente tous les processus biologiques de ton corps. En 1988, l'immunologiste français Dr. Jacques Benveniste, a démontré que l'eau a une mémoire.. Il a démontré que l'eau pouvait conserver la signature électromagnétique d'une substance, même après que cette substance ait été complètement diluée hors d'elle.. L'eau se souvenait de la fréquence, il a publié ses découvertes dans Nature — la revue scientifique la plus prestigieuse de la Terre. En quelques mois, le financement de son laboratoire a été coupé.... Sa réputation a été détruite, sa carrière terminée...!!! Pourquoi ? Parce que si l'eau peut stocker et transmettre de la fréquence, alors toute la fondation de la médecine chimique s'effondre.. Si tes cellules sont pleines de cristaux liquides qui répondent aux signaux électromagnétiques, tu n'as pas besoin d'une pilule chimique pour changer ta biologie, tu auras juste besoin de la bonne fréquence. Maintenant regarde ce qu'ils ont fait à ton eau.. Ils la font passer à travers des kilomètres de tuyaux métalliques sous pression, ils l'inondent de chlore... Ils ajoutent du fluorure, ils la privent de tout minéral et de toute structure naturelle qu'elle contenait autrefois.. Quand elle arrive dans ton verre, elle est électromagnétiquement morte..!!! Tu es 70% d'eau, mais pas leur eau, ton corps a été conçu pour fonctionner avec des cristaux liquides structurés, cohérents et sensibles à la fréquence.. Et ils se sont assurés, que tu n'y aies jamais accès !!! La médecine quantique ne traite pas les symptômes.. Elle restaure le signal. Elle répare l'eau, elle répare la fréquence, et le corps se souvient comment guérir..

A neurobiologist at Columbia spent 30 years proving that the gut has its own brain, and the day he finally published the book that named it, almost every psychiatrist in America stopped returning his calls. His name is Michael Gershon. He runs the Department of Anatomy and Cell Biology at Columbia University Medical Center in New York, and the field he built from the ground up is called neurogastroenterology in short brain-gut axis. The book that announced it to the world was published in 1998, and the title alone tells you everything about what he was up against. He called it The Second Brain. The claim sounded like science fiction in the 1990s. Gershon was saying that the human gut contains its own fully functional nervous system, with around 100 million neurons embedded in the walls of the alimentary canal, which is the nine-meter tube running from your esophagus to your anus. That is more neurons than your entire spinal cord, and more than your entire peripheral nervous system put together. The gut was not just digesting food. It was running its own intelligence, with its own reflexes, its own memory, and its own way of deciding what to do without asking the brain in your head for permission. The medical establishment treated this as borderline heretical when he first started publishing it. The brain was supposed to be the command center. Everything else was supposed to be the periphery. A second brain in the belly did not fit the architecture anyone had been taught. Then the data started piling up, and it was impossible to argue with. The first finding that broke the old model was about serotonin. You might have heard Andrew Huberman talking about it on his podcasts. Serotonin is the neurotransmitter associated with mood, well-being, sleep, and depression. Every antidepressant on the market targets it. The assumption for decades was that serotonin was a brain chemical, produced in the brain, regulated in the brain, and responsible for what happened inside the brain. Gershon's lab showed that 90 to 95 percent of the body's serotonin is not produced in the brain at all. It is produced in the gut, by specialized cells called enterochromaffin cells embedded in the intestinal lining. Your stomach and intestines are the largest serotonin factory in the human body, and the brain in your skull is producing only a tiny fraction of what is circulating below your neck. The second finding was even harder to swallow. The vagus nerve is the longest cranial nerve in the body, running from the base of the brain down through the neck, the chest, and into the abdomen, where it branches into the gut. For most of the 20th century, doctors assumed the vagus was the brain's way of giving orders to the digestive system, in the same way the brain gives orders to the rest of the body. The actual measurements showed almost the opposite. Roughly 90 percent of the fibers in the vagus nerve are carrying signals upward, from the gut to the brain, and only a small fraction are carrying signals downward. Your gut is sending nine times more information to your head than your head is sending to your gut. The bandwidth is wildly asymmetrical, and almost all of it is going in a direction the medical textbooks had quietly been wrong about for decades. The implication of those two findings together is what changed psychiatry. If most of your serotonin is being produced in your gut, and most of the information flowing through your vagus nerve is moving from your gut to your brain, then your mood is being shaped from the bottom up far more than it is being directed from the top down. The feeling of dread before a difficult meeting. The sudden clarity after a good meal. The low-grade anxiety that will not go away no matter how much you talk through it. All of it is downstream of signals that started below your diaphragm. A 2019 study at McMaster University put the final piece in place. Researchers gave mice oral antidepressants and watched what happened. The drugs activated the vagus nerve from the gut side, and the gut-to-brain signaling was what produced the antidepressant effect. When they cut the vagus nerve and tried the same drugs, the antidepressant effect disappeared completely. The drug was not working on the brain directly. It was working on the gut, and the gut was working on the brain. The follow-up research on the microbiome made the connection even tighter. Mice raised in completely sterile environments with no gut bacteria produced about 60 percent less serotonin in their intestines than normal mice. When the bacteria were reintroduced, serotonin production returned to normal. The trillions of microorganisms living in your digestive tract are not passengers. They are running the factory that makes the chemical your antidepressant is trying to manipulate. The most haunting line from Gershon's interviews is the one I keep coming back to. He said the second brain does not do philosophy or poetry, and it cannot help you write a novel. But it is the brain that decides whether you wake up in the morning feeling like the day is full of possibility or feeling like something is wrong before anything has even happened. The mood you assume your conscious mind is generating from your thoughts is mostly being generated underneath you, by a nervous system you cannot feel and cannot consciously access, in an organ you have spent your entire life thinking about as a digestion machine. The decision your gut makes about how you are going to feel arrives in your head a fraction of a second before your brain catches up to it. The conscious thought is the explanation your mind invents for a verdict that has already been reached somewhere lower. You did not feel uneasy because you were thinking dark thoughts. You started thinking dark thoughts because your gut was already uneasy.

🚨🇳🇬💀LES CHRÉTIENS DU NIGERIA RESPIRENT: LE BOUCHER DE L’ÉTAT ISLAMIQUE EST MORT Trump annonce que les forces US ont buté le N°2 de l’Etat Islamique au Nigeria : Abu-Bilal al-Minuki. « Il ne tuera plus de chrétiens ni ne préparera d’attentats contre nous. » Opération propre, sources infiltrées, et résultat immédiat. L’EI vient de prendre un sacré coup dans la gueule.

DES LÉGUMES QUI PEUVENT POUSSER SANS LUMIÈRE DIRECTE "L'ombre n'est pas l'ennemi de la croissance des plantes. Ce sont juste des conditions différentes auxquelles certaines plantes sont adaptées. Tous les jardins ne sont pas conçus idéalement en plein soleil. Cela n'empêche pas de cultiver. Il suffit d'adapter les plantes semées. Les épinards : étaient déja cultivées en Perse il y a de nombreux siècles, dans des cours fraîches et ombragées. Exposés au soleil de l'après midi, ils montent en graines, accélérent vers leur floraison et deviennent amers. L'Ombre ralentit ce processus. La laitue : n'aime pas la chaleur. A l'ombre elle étend ses feuilles plus largement. Pousse plus lentement mais plus régulièrement. Et la fenêtre de récolte est plus longue que pour celles plantées au soleil. La roquette. En plein soleil, elle monte en graines rapidement. A l'ombre, elle est conçue pour' pousser régulièrement. Les petits pois. Une autre culture de saison fraîche. Ils perdent leurs fleurs si le soleil est fort et direct. Pas de fleurs, pas de gousses. Le choix frisé. Une ancienne culture de survie résiliente. Il tolère l'ombre partielle maintenant une croissance régulière même avec 3 heures de lumière indirectes par jour. La bette à cardes. Elle prospère avec un ensoleillement réduit, de 2 à 4 heures d'ensoleillement indirect par jour. L'ail. A l'ombre il pousse plus lentement mais plus gros et avec plus de saveur. Il est moins dépendant de la photosynthèse que beaucoup de plantes. Les carottes. A l'origine c'était une culture de vallées partiellement ombragées. A l'ombre les racines sont souvent supérieures en texture et en saveur. La menthe. La plus tolérante à l'ombre des plantes aromatiques. La coriandre. Elle monte en graines rapidement au soleil direct et avec la chaleur. Le pak Choi Originaire de vallées Chinoises ombragées. Le cresson de fontaines. Souvent plantés sur les berges ombragées des ruisseaux. Peu d'entretien et produit en continu. Les champignons. Comme les shiitake. Les pleurotes. Le soleil stoppe leur croissance. Sur des lits de paille ou des bûches. La mâche. Elle pousse très bien même en pleine ombre et résistante au froid. L'oseille. Une plante vivace qui tolère l'ombre et les sols pauvres. Endive et chicorée Elles prospèrent à l'ombre partielle ou totale. Cultivée intentionnellement dans l'obscurité complète depuis 1830. L'égopode. Une ancienne plante cultivée dans les monastères du moyen-âge qui prospère à l'ombre. #jardin #garden #plantes #plants Merci https://t.co/aHb88rgnbk

They have kept these amazing natural cures from us 😔 A 4-month-old baby diagnosed with stage 4 liver cancer… parents refused chemo and healed her completely with chlorine dioxide (CDS) baths: 100 drops in the tub morning AND night (30 minutes each). She’s now a healthy, thriving 7-year-old — even taller than her peers! Mark Grenon shares this powerful story (the same man they jailed along with his sons for helping people worldwide with this remedy). Natural healing is real. Watch till the end

🚨 L’IMPORTANCE DES FRÉQUENCES : NOUS RÉSONNONS AVEC LA NATURE 🌿🔊 😱❗Regardez cette démonstration simple mais puissante : 💥Un diapason à 512 Hz est frappé à côté d’un diapason à 440 Hz. Même sans contact direct, les vibrations se transmettent et créent une résonance. Nous possédons tous des fréquences naturelles sur lesquelles nous vibrons en permanence. Lorsque nous utilisons ces fréquences en harmonie avec la nature, elles attirent et amplifient. C’est exactement pour cela que ces fréquences sont aussi les fréquences naturelles de la Terre et du vivant. Nous avons besoin de nous reconnecter. C’est le vrai sens de se relier à Mère Nature.

A Russian biophysicist spent 30 years proving that shining red light on a cell could double its energy, and almost nobody believed her until a tech billionaire named Bryan Johnson made her work the most searched biohack on the internet. Her name was Tiina Karu. She worked in a Moscow lab through the 1980s and 1990s, and the discovery she defended for decades sat in journals nobody read while the rest of medicine ignored her. The whole thing started by accident. In 1967, a Hungarian doctor named Endre Mester was trying to use a new device called a laser to burn tumors out of mice. His laser was broken. It did not have enough power to burn anything. He used it anyway. The mice grew their hair back faster than the control group. Their wounds healed faster too. He had no idea why. Tiina Karu picked up his work and asked the question that mattered. Why does this happen. She ran experiments for 20 years. Different wavelengths. Different doses. Measuring what happens inside the cell when red light hits it. The answer she landed on was almost too specific to be true. The thing in your body that responds to red light is one enzyme. Cytochrome c oxidase. It sits inside your mitochondria. Mitochondria are the part of your cell that makes energy. They take oxygen and food and turn it into a molecule called ATP, which is the fuel your cells run on. Your body makes 40 to 70 kilograms of ATP every single day just to keep you alive. If your mitochondria slow down, you age faster, heal slower, lose hair, lose muscle, and get inflamed easier. Cytochrome c oxidase does most of the work. It contains copper and iron atoms. Those atoms happen to absorb light at very specific colors. Red light at 630 to 670 nanometers. Near-infrared light at 810 to 850 nanometers. Other colors do almost nothing. Blue does not work. Green does not work. The biology is locked to those two windows because that is what the metal inside the enzyme can physically catch. When a red photon hits that enzyme, three things happen. The enzyme runs faster. ATP production jumps 30 to 40% within minutes. Nitric oxide gets released. Blood vessels widen. More oxygen and nutrients flow in. A small stress signal goes off inside the cell that tells it to repair itself. The same signal it gets after exercise. Red light is not adding anything to the cell. It is just unlocking work the cell was already trying to do. For 30 years almost nobody outside her field cared. Red light therapy lived inside dental clinics for mouth ulcers and physical therapy offices for tendonitis. Medical schools did not teach it. The science sat in obscure journals. Then the evidence started piling up. A 2024 review of 18 trials confirmed red light speeds up wound healing. Another 2024 review found it lowered inflammation markers by 38% over 4 weeks. Athletes using red light before training had 45% less muscle soreness the next day. Seven separate trials on hair loss showed visible regrowth in every single one. A 2024 study found 15 minutes of red light before a meal cut blood sugar spikes by 27.7%. In March 2026, Nature published a 4,000 word feature on red light therapy. The most respected scientific journal on Earth officially admitted there was real biology under the hype. That was the moment the field crossed from fringe to mainstream. Bryan Johnson is the reason the average person now knows any of this exists. He uses a red light cap on his scalp for 6 minutes daily and a full-body panel three times a week. He posted his hair regrowth photos and his skin scans, and the algorithm did the rest. Red light masks went from biohacker forums to Sephora shelves in two years. Tiina Karu died in 2019. She did not live to see Nature validate her. She did not live to see a billionaire turn the enzyme she identified into a billion dollar industry. Every red light mask, panel, cap, and bed on the planet right now is just a way to deliver the photons she proved mattered. The wavelengths were always there. The enzyme was always there. The biology was always real. It just took a Hungarian doctor with a broken laser, a Russian scientist nobody listened to, and one tech billionaire willing to stand in front of a glowing panel for the world to finally pay attention.