大狼毒根茎中对胰腺癌SW1990细胞具有毒性的二萜

采用硅胶柱色谱、MCI柱色谱、Sephadex LH-20柱色谱和半制备高效液相色谱等分离方法对大狼毒根茎的化学成分进行研究,通过高分辨电喷雾电离质谱(HR-ESI-MS)、核磁共振(NMR)和计算电子圆二色谱(ECD)等方法鉴定了8个二萜类成分,包括2个新的对映松香烷型二萜类化合物(1~2)、4个已知对映松香烷型二萜(3~6)和2个已知续随子烷型二萜(7~8).(7R,8S)-7,8-二羟基-17-降碳对映松香烷-13(14)-烯-15-酮(1)为C-17位降碳的松香烷型二萜类成分,化合物2为松香烷型二萜内酯类成分.细胞毒活性筛选表明,化合物7对胰腺癌SW1990细胞具有明显的毒性,IC50为(44.97±9.16)μmol/L;并且能剂量依赖性地促进SW1990细胞的前期凋亡,通过降低胰腺癌细胞内抑制凋亡蛋白Bcl-2的表达发挥抑制肿瘤细胞作用.

Fluffy hybrid nanoadjuvants for reversing the imbalance of osteoclastic andosteogenic niches in osteoporosis

Osteoporosis is majorly caused by an imbalance between osteoclastic and osteogenic niches. Despite thedevelopment of nationally recognized first-line anti-osteoporosis drugs, including alendronate (AL), their lowbioavailability, poor uptake rate, and dose-related side effects present significant challenges in treatment. Thiscalls for an urgent need for more effective bone-affinity drug delivery systems. In this study, we produced hybridstructures with bioactive components and stable fluffy topological morphology by cross-linking calcium andphosphorus precursors based on mesoporous silica to fabricate nanoadjuvants for AL delivery. The subsequentgrafting of -PEG-DAsp8 ensured superior biocompatibility and bone targeting capacity. RNA sequencing revealedthat these fluffy nanoadjuvants effectively activated adhesion pathways through CARD11 and CD34 molecularmechanisms, hence promoting cellular uptake and intracellular delivery of AL. Experiments showed that smalldoseAL nanoadjuvants effectively suppress osteoclast formation and potentially promote osteogenesis. In vivoresults restored the balance between osteogenic and osteoclastic niches against osteoporosis as well as theconsequent significant recovery of bone mass. Therefore, this study constructed a drug nanoadjuvant withpeculiar topological structures and high bone targeting capacities, efficient intracellular drug delivery as well asbone bioactivity. This provides a novel perspective on drug delivery for osteoporosis and treatment strategies forother bone diseases.

Durable immunomodulatory hierarchical patch for rotator cuff repairing

Degradable rotator cuff patches,followed over five years,have been observed to exhibit high re-tear rates exceeding 50%,which is attributed to the inability of degradable polymers alone to restore the post-rotator cuff tear(RCT)inflammatory niche.Herein,poly(ester-ferulic acid-urethane)urea(PEFUU)was developed,featuring prolonged anti-inflammatory functionality,achieved by the integration of ferulic acid(FA)into the polyurethane repeating units.PEFUU stably releases FA in vitro,reversing the inflammatory niche produced by M1 macrophages and restoring the directed differentiation of stem cells.Utilizing PEFUU,hierarchical composite nanofiber patch(HCNP)was fabricated,simulating the natural microstructure of the tendon-to-bone interface with an aligned-random alignment.The incorporation of enzymatic hydrolysate derived from decellularized Wharton jelly tissue into the random layer could further enhance cartilage regeneration at the tendon-to-bone interface.Via rat RCT repairing model,HCNP possessing prolonged anti-inflammatory properties uniquely facilitated physiological healing at the tendon-to-bone interface’s microstructure.The alignment of fibers was restored,and histologically,the characteristic tripartite distribution of collagen I-collagen II-collagen I was achieved.This study offers a universal approach to the functionalization of degradable polymers and provides a foundational reference for their future applications in promoting the in vivo regeneration of musculoskeletal tissues.