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Chiba University Dec 16 2024

Craniopharyngiomas are brain tumors that negatively impact the hormonal function of the nearby pituitary. The tumor location often prevents necessary surgical intervention. Alternative pharmacological therapy requires an in-depth understanding of the tumor molecular characteristics. To address this gap, researchers from Japan analyzed gene expression within individual tumor cells. This study reports the molecular features and interactions of tumor and immune cells associated with two craniopharyngioma subtypes that will help identify future targeted therapeutics.

Craniopharyngioma (CP) is a rare brain tumor that develops in the regions close to the hypothalamus and pituitary gland. The CP tumors lead to complications like defective vision, neuronal defects, diabetes, and developmental problems. There are two primary subtypes of CPs: adamantinomatous craniopharyngioma (ACP) and papillary craniopharyngioma (PCP). These two subtypes are distinguished by their distinct genetic profiles. ACP is typically characterized by mutations in the CTNNB1 gene, while PCP is primarily associated with BRAF gene mutations.

The primary course of action for treating CP is surgical intervention. However, the tumor's invasive nature and its location near critical structures present a significant challenge in terms of surgical intervention. As the tumor progresses, it infiltrates the surrounding tissue, resulting in significant neurological impairments. Therefore, surgery alone is insufficient to address the complex challenges posed by CPs. It is essential to have a comprehensive understanding of the tumor's biological characteristics and molecular progression in order to ensure successful tumor extraction while preserving surrounding healthy tissue.

Against this backdrop, Professor Tomoaki Tanaka collaborated with Professor Yoshinori Higuchi and Dr. Takashi Kono from the Graduate School of Medicine at Chiba University in Japan to conduct a study to elucidate the underlying biological processes involved in this tumor. The study was made available online on September 30, 2024, and was published in Volume 27 Issue 11 of the journal iScience on November 15, 2024.

To this end, they utilized single-cell RNA sequencing, a technique that reveals differences in gene expression across individual cells, and analyzed 10 cases of CPs.

In an interview, Prof. Tanaka, the senior author of the study, explained the motivation behind it. He said, "Despite being histologically benign, these tumors can significantly impact critical brain structures." "Our goal was to develop more targeted and less invasive therapeutic approaches that could significantly improve patient outcomes and quality of life."

The single-cell analysis revealed a diverse range of cell types within the tumor microenvironment (TME), including tumor cells, immune cells, and fibroblasts, with varying proportions across cases. The tumor cells were classified into two main subtypes: Type 1, which is predominant in ACP, and Type 2, which is dominant in PCP. The single-cell gene expression data from the ACP and PCP subtypes was clustered to reveal distinct cell types within the tumors. The study identified cell types linked to the development of epithelial cells and the immune response in both ACP and PCP tumors. However, the cell types involved in tumor calcification were particularly prevalent in ACP, while the cell cycle-associated genes were predominant in the PCP type.

Further, the research team observed a notable diversity in macrophage types between the two tumor types. The pro-inflammatory M1 macrophages and inflammation-related markers were found to be higher in ACP, while the anti-inflammatory M2 macrophages were higher in PCP. Accordingly, a higher ratio of M1 and M2 macrophages was correlated with the occurrence of diabetes and pituitary insufficiency.

Additionally, the study identified a prominent cell-cell interaction between cell surface proteins CD44-secreted phosphoprotein 1 (SPP1). This SPP1-CD44 signal from classical M2 inhibited the sustained proliferation of T cells.

This study presents a comprehensive map of cell types within CP tumors and reports a significant relationship between immune cells and clinical symptoms.

Prof. Tanaka highlighted the clinical implications of their findings, stating, "These findings open up the possibility of personalized treatment approaches for patients with CP based on their specific tumor subtype and immune cell composition. Understanding these differences will also assist clinicians in predicting which patients are at higher risk for complications like diabetes insipidus."

Going ahead, these findings can enable the creation of new targeted therapies that precisely influence the tumor microenvironment and immune cell interactions, ultimately leading to more effective treatments with reduced adverse effects.

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Chiba UniversityJournal reference:

Matsuda, T., et al. (2024). Deciphering craniopharyngioma subtypes: Single-cell analysis of tumor microenvironment and immune networks. iScience. doi.org/10.1016/j.isci.2024.111068.

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Sources: BoSox send rookie Campbell to minors

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Sources: BoSox send rookie Campbell to minors

The Boston Red Sox are sending rookie Kristian Campbell to Triple-A, paving the way for the return of outfielder Wilyer Abreu off the injured list, sources told ESPN on Thursday.

Campbell, the reigning Minor League Player of the Year, signed an eight-year, $60 million contract extension before the beginning of the season and won American League Rookie of the Month in April, hitting .301/.407/.495. Since May, he has struggled offensively, hitting .159/.243/.222, and defensively as the Red Sox’s everyday second baseman.

The reset for Campbell, who turns 23 on June 28, comes in the wake of Boston trading star slugger Rafael Devers to the San Francisco Giants. The return of Abreu and eventual return of third baseman Alex Bregman from a right quadriceps strain are expected to fortify a lineup that ranks fifth in the major leagues with 358 runs scored.

Campbell rocketed to the big leagues after a 2024 in which he hit .330/.439/.558 with 20 home runs and 77 RBIs over three minor league levels. Boston entered spring training hopeful he would earn the second base job, and despite hitting .167/.305/.271, the Red Sox were confident enough in Campbell’s ability to succeed that they locked him up to a deal that with two club options can run through 2034.

With a unique stance, Campbell managed to produce top-end exit velocities, and the Red Sox banked on that ability to make up for his lack of minor league at-bats. A fourth-round pick out of Georgia Tech in 2023, the 6-foot-3, 210-pound Campbell responded with four multihit games among his first seven in the big leagues and finished April with four home runs and 12 RBIs.

May and June have proven far more difficult, with just four multihit games among the 38 he has played. Campbell spent the first eight days of May in the cleanup spot but has been dropped to the bottom of the order in June. In his last big league game Wednesday, he batted eighth and played center field.

Abreu, who turns 26 on Tuesday, is expected to rejoin the Red Sox 10 days after hitting the injured list with a strained oblique. He went 1 for 4 in a rehabilitation appearance with Triple-A Worcester on Tuesday and would head to San Francisco for the Red Sox’s series against the Giants that begins Friday.

In his third big league season, Abreu is hitting .245/.321/.471 with 13 home runs, just two shy of his career best in 2024. He joins a crowded outfield, with Gold Glove candidate Ceddanne Rafaela — who can also play in the middle infield — in center, All-Star Jarren Duran in left and top prospect Roman Anthony in right. Anthony is currently hitting third, the spot Abreu regularly occupied before his injury.

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Jac jack: Royals’ Caglianone belts first MLB HR

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Jac jack: Royals' Caglianone belts first MLB HR

ARLINGTON, Texas — Jac Caglianone has his first career home run just shy of two weeks after his debut with the Kansas City Royals, and a day after the 22-year-old prospect sat out of a big league game for the first time.

Caglianone won a lefty-lefty matchup by pulling a 95.5 mph fastball from Jacob Latz into the Texas Rangers bullpen in right-center field to give the Royals a 3-0 lead in the second inning Thursday.

Vinnie Pasquantino hit a two-run shot off Texas starter Shawn Armstrong in the first inning of a bullpen game for the Rangers.

The sixth overall pick in last year’s amateur draft out of Florida, Caglianone went 0-for-5 in his big league debut at St. Louis on June 3. His average was at .196 after going 0-for-4 in the opener of a series at Texas and sitting out the second game.

Caglianone, who played his first six games on the road before making his home debut against the New York Yankees, swung at Latz’s 2-2 pitch above the strike zone, and pointed toward center field as he rounded second base after his 387-foot drive.

The 6-foot-5 Caglianone hit 15 homers in 50 games combined with Double-A Northwest Arkansas and Triple-A Omaha before getting called up.

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Ohtani to pitch against Nationals on Sunday

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Ohtani to pitch against Nationals on Sunday

LOS ANGELES — Shohei Ohtani will next pitch for the Los Angeles Dodgers on Sunday against the Washington Nationals.

The two-way superstar made his mound debut for the Dodgers on Monday against the San Diego Padres, throwing one inning and allowing one run and two hits. He also batted leadoff as the designated hitter and had two hits.

Ohtani faced Padres sluggers Fernando Tatis Jr. and Manny Machado in his 28-pitch outing.

The Dodgers conclude their four-game series with San Diego on Thursday night, looking for a sweep and their sixth straight victory.

Ohtani underwent Tommy John surgery after the 2023 season while with the Los Angeles Angels and missed all of the 2024 season after which he signed a $700 million, 10-year deal with the Dodgers.

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