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CANCER HAS BEEN CURED Ivermectin & Fenbendazole cure cancer. Pass it on. BREAKING NEWS: First-in-the-World Ivermectin, Mebendazole and Fenbendazole Protocol in Cancer has been peer-reviewed and published on Sep.19, 2024! The future of Cancer Treatment starts NOW. My thanks to lead authors Ilyes Baghli and Pierrick Martinez for their incredible inspired work, FLCCC’s Dr.Paul Marik for his extensive work on repurposed drugs and every co-author who worked hard to bring this paper to life. I hope that this peer-reviewed paper lays the groundwork for a brand new future for Cancer Treatment. Many of you know that I have been helping thousands of Cancer patients with high dose Ivermectin, Mebendazole, and Fenbendazole FOLLOW ME, THE NEXT DROP WILL BE SHOCKING

The peptides that helped me transform in 11 months: 1)Retatrutide(glp3) 2)Melanotan-2 3)Mots-c 4)BPC-157 5)TB-500 6)KPV 7)Glutathione 8)Thymosin Alpha 1 9)GHK-Cu 10)CJC1295 11)Ipamorelin These are all peptides that I have tried, many of which I wouldn’t run again and are very situational. Few are ran year around. L’chaim to a year of more peptides https://t.co/Z37ZJl2szP code AALEX for 10% off of the peps that use

🚨 THE “HORSE DEWORMER” THEY MOCKED JUST HIT 25 MILLION VIEWS IN DAYS People are paying attention again. Not because of headlines. Not because of pharma ads. Not because TV told them to. Because people are searching for answers themselves. Why Ivermectin keeps coming back into the conversation: ✅ Nobel Prize winning discovery in 2015 for parasitic disease research. ✅ Decades of worldwide human use ✅ Massive public interest in repurposed medicine ✅ Millions openly discussing personal experiences online And the biggest reason? People feel like the public conversation around affordable repurposed drugs was shut down instead of openly debated. Whether critics like it or not: The internet is FULL of people sharing stories, protocols, questions, and experiences. But it does prove one thing: The public never stopped searching for alternatives.

CANCER HAS BEEN CURED Ivermectin & Fenbendazole cure cancer. Pass it on. BREAKING NEWS: First-in-the-World Ivermectin, Mebendazole and Fenbendazole Protocol in Cancer has been peer-reviewed and published on Sep.19, 2024! The future of Cancer Treatment starts NOW. My thanks to lead authors Ilyes Baghli and Pierrick Martinez for their incredible inspired work, FLCCC’s Dr.Paul Marik for his extensive work on repurposed drugs and every co-author who worked hard to bring this paper to life. I hope that this peer-reviewed paper lays the groundwork for a brand new future for Cancer Treatment. Many of you know that I have been helping thousands of Cancer patients with high dose Ivermectin, Mebendazole, and Fenbendazole

Penis size is set before birth by maternal health, metabolism, and hormone exposure (including birth control) Penis size is largely determined during fetal development through the maternal–placental endocrine system. Masculinization depends on DHT acting locally in genital tissue. Fetal circulating DHT is often very low, which shows that the androgenic signal is generated inside tissues from precursors rather than delivered directly through blood. A major part of this signal comes from the backdoor pathway. Placental progesterone is converted across fetal tissues into intermediates such as androsterone, which are then converted locally into DHT in target organs. This pathway bypasses testosterone as an obligatory step. The placenta provides a continuous supply of progesterone derived from maternal cholesterol, so androgen production depends on maternal substrate availability and its processing across fetal liver, adrenal glands, and peripheral tissues. The system is distributed and depends on coordinated enzymatic activity rather than a single endocrine source. Conversion efficiency depends on metabolic conditions. Thyroid function, mitochondrial activity, oxygen availability, and stress signaling determine whether progesterone is efficiently converted into androgenic intermediates or diverted toward other pathways. Maternal endocrine state directly modifies these conditions. Hormonal contraceptives suppress endogenous progesterone production, alter estrogen signaling, and modify stress-axis regulation, replacing a cyclical endocrine pattern with a static pharmacological one. This changes substrate dynamics, timing, and pathway organization during fetal development. Synthetic progestins are not equivalent to physiological progesterone. They activate receptors but do not function as interchangeable substrates within steroidogenesis, so downstream androgen and neurosteroid pathways are altered. Puberty mainly amplifies androgen exposure and completes growth. The structural baseline is established earlier through progesterone availability, metabolic capacity, enzyme expression, and local DHT production shaped by the maternal environment.